Your search keyword '"Reed EC"' showing total 101 results

1. Lymphocyte reconstitution after allogeneic blood stem cell transplantation for hematologic malignancies

Author

Pavletic, ZS, Joshi, SS, Pirruccello, SJ, Tarantolo, SR, Kollath, J, Reed, EC, Bierman, PJ, Vose, JM, Warkentin, PI, Gross, TG, Nasrati, K, Armitage, JO, Kessinger, A, and Bishop, MR

Published

1998

2. Centrality, rapidity and transverse momentum dependence of J/ψ suppression in Pb–Pb collisions at √sNN = 2.76 TeV

Author

Piano, Stefano, Lea, Ramona, Camerini, Paolo, Luparello, Grazia, Fragiacomo, Enrico, Margagliotti, Giacomo, Rui, Rinaldo, Abelev bv, B., Adam al, J., Adamová cd, D., Aggarwal ch, M. M., Aglieri Rinella ah, G., Agnello cn, M., Agocs eb, A. G., Agostinelli z, A., Agrawal as, N., Ahammed dx, Z., Ahmad r, N., Ahmad Masoodi r, A., Ahmed o, I., Ahn bo, S. U., Ahn bo, S. A., Aimo de, I., Aiola ec, S., Ajaz o, M., Akindinov be, A., Aleksandrov ct, D., Alessandro de, B., Alexandre cv, D., Alici l, A., Alkin c, A., Alme aj, J., Alt an, T., Altini ae, V., Altinpinar q, S., Altsybeev dw, I., Alves Garcia Prado dm, C., Andrei by, C., Andronic cq, A., Anguelov cm, V., Anielski az, J., Anticˇic ́ cr, T., Antinori db, F., Antonioli cy, P., Aphecetche df, L., Appelshäuser ax, H., Arbor br, N., Arcelli z, S., Armesto p, N., Arnaldi de, R., Aronsson ec, T., Arsene u, I. C., Arslandok ax, M., Augustinus ah, A., Averbeck cq, R., Awes ce, T. C., Azmi r, M. D., Bach an, M., Badalà da, A., Baek ao, Y. W., Bagnasco de, S., Bailhache ax, R., Bairathi cl, V., Bala ck, R., Baldisseri n, A., Baltasar Dos Santos Pedrosa ah, F., Bán bf, J., Baral bh, R. C., Barbera aa, R., Barile ae, F., Barnaföldi eb, G. G., Barnby cv, L. S., Barret bq, V., Bartke dj, J., Basile z, M., Bastid bq, N., Basu dx, S., Bathen az, B., Batigne df, G., Batyunya bm, B., Batzing u, P. C., Baumann ax, C., Bearden ca, I. G., Beck ax, H., Bedda cn, C., Behera as, N. K., Belikov ba, I., Bellini z, F., Bellwied do, R., Belmont Moreno bk, E., Bencedi eb, G., Beole y, S., Berceanu by, I., Bercuci by, A., Berdnikov cf, Y., 1, Berenyi eb, D., Berger di, M. E., Bergognon df, A. A. E., Bertens bd, R. A., Berzano y, D., Betev ah, L., Bhasin ck, A., Bhati ch, A. K., Bhattacharjee ap, B., Bhom dt, J., Bianchi y, L., Bianchi bs, N., Bianchin bd, C., Bielcˇík al, J., Bielcˇíková cd, J., Bilandzic ca, A., Bjelogrlic bd, S., Blanco j, F., Blau ct, D., Blume ax, C., Bock bu, F., Boehmer di, F. V., Bogdanov bw, A., Bøggild ca, H., Bogolyubsky bb, M., Boldizsár eb, L., Bombara am, M., Book ax, J., Borel n, H., Borissov cp, A., Bornschein an, J., Bossú bl, F., Botje cb, M., Botta y, E., Böttger aw, S., Braun Munzinger cq, P., Bregant dm, M., Breitner aw, T., Broker ax, T. A., Browning co, T. A., Broz ak, M., Bruna de, E., Bruno ae, G. E., Budnikov cs, D., Buesching ax, H., Bufalino de, S., Buncic ah, P., Busch cm, O., Buthelezi bl, Z., Caffarri ab, D., Cai g, X., Caines ec, H., Caliva bd, A., Calvo Villar cw, E., Canoa Roman ah, V., Carena ah, F., Carena ah, W., Carminati ah, F., Casanova Díaz bs, A., Castillo Castellanos n, J., Casula w, E. A. R., Catanescu by, V., Cavicchioli ah, C., Ceballos Sanchez i, C., Cepila al, J., Cerello de, P., Chang dp, B., Chapeland ah, S., Charvet n, J. L., Chattopadhyay dx, S., Chattopadhyay cu, S., Cherney cg, M., Cheshkov dv, C., Cheynis dv, B., Chibante Barroso ah, V., Chinellato do, D. D., Chochula ah, P., Chojnacki ca, M., Choudhury dx, S., Christakoglou cb, P., Christensen ca, C. H., Christiansen af, P., Chujo dt, T., Chung cp, S. U., Cicalo cz, C., Cifarelli l, L., Z, Cindolo cy, F., Cleymans cj, J., Colamaria ae, F., Colella ae, D., Collu w, A., Colocci z, M., Conesa Balbastre br, G., Conesa del Valle av, Z., Connors ec, M. E., Contin x, G., Contreras k, J. G., Cormier ce, T. M., Corrales Morales y, Y., Cortese ad, P., Cortés Maldonado b, I., Cosentino bu, M. R., Costa ah, F., Crochet bq, P., Cruz Albino k, R., Cuautle bj, E., Cunqueiro bs, L., Dainese db, A., Dang g, R., Danu bi, A., Das cu, D., Das av, I., Das cu, K., Das d, S., Dash dn, A., Dash as, S., De dx, S., Delagrange df, H., 2, Deloff bx, A., Dénes eb, E., D’Erasmo ae, G., de Barros dm, G. O. V., De Caro l, A., de Cataldo cx, G., de Cuveland an, J., De Falco w, A., De Gruttola ac, D., L, De Marco de, N., De Pasquale ac, S., de Rooij bd, R., Diaz Corchero j, M. A., Dietel az, T., Divià ah, R., Di Bari ae, D., Di Liberto dc, S., Di Mauro ah, A., Di Nezza bs, P., Djuvsland q, Ø., Dobrin bd, A., Dobrowolski bx, T., Domenicis Gimenez dm, D., Dönigus ax, B., Dordic u, O., Dorheim di, S., Dubey dx, A. K., Dubla bd, A., Ducroux dv, L., Dupieux bq, P., Dutta Majumdar cu, A. K., Elia cx, D., Engel aw, H., Erazmus ah, B., Erdal aj, H. A., Eschweiler an, D., Espagnon av, B., Estienne df, M., Esumi dt, S., Evans cv, D., Evdokimov bb, S., Eyyubova u, G., Fabris db, D., Faivre br, J., Falchieri z, D., Fantoni bs, A., Fasel cm, M., Fehlker q, D., Feldkamp az, L., Felea bi, D., Feliciello de, A., Feofilov dw, G., Ferencei cd, J., Fernández Téllez b, A., Ferreiro p, E. G., Ferretti y, A., Festanti ab, A., Figiel dj, J., Figueredo dm, M. A. S., Filchagin cs, S., Finogeev bc, D., Fionda ae, F. M., Fiore ae, E. M., Floratos ci, E., Floris ah, M., Foertsch bl, S., Foka cq, P., Fokin ct, S., Francescon ab, A., Frankenfeld cq, U., Fuchs ah, U., Furget br, C., Fusco Girard ac, M., Gaardhøje ca, J. J., Gagliardi y, M., Gallio y, M., Gangadharan s, D. R., Ganoti ce, P., Garabatos cq, C., Garcia Solis m, E., Gargiulo ah, C., Garishvili bv, I., Gerhard an, J., Germain df, M., Gheata ah, A., Gheata ah, M., Ghidini ae, B., Ghosh dx, P., Ghosh d, S. K., Gianotti bs, P., Giubellino ah, P., Gladysz Dziadus dj, E., Glässel cm, P., Gomez k, R., González Zamora j, P., Gorbunov an, S., Görlich dj, L., Gotovac dh, S., Graczykowski dz, L. K., Grajcarek cm, R., Grelli bd, A., Grigoras ah, A., Grigoras ah, C., Grigoriev bw, V., Grigoryan a, A., Grigoryan bm, S., Grinyov c, B., Grion dd, N., Grosse Oetringhaus ah, J. F., Grossiord dv, J. Y., Grosso ah, R., Guber bc, F., Guernane br, R., Guerzoni z, B., Guilbaud dv, M., Gulbrandsen ca, K., Gulkanyan a, H., Gunji ds, T., Gupta ck, A., Gupta ck, R., Khan o, K. H., Haake az, R., Haaland q, Ø., Hadjidakis av, C., Haiduc bi, M., Hamagaki ds, H., Hamar eb, G., Hanratty cv, L. D., Hansen ca, A., Harris ec, J. W., Hartmann an, H., Harton m, A., Hatzifotiadou cy, D., Hayashi ds, S., Hayrapetyan ah, A., A, Heckel ax, S. T., Heide az, M., Helstrup aj, H., Herghelegiu by, A., Herrera Corral k, G., Hess ag, B. A., Hetland aj, K. F., Hicks ec, B., Hippolyte ba, B., Hladky bg, J., Hristov ah, P., Huang q, M., Humanic s, T. J., Hutter an, D., Hwang t, D. S., Ianigro dv, J. C., Ilkaev cs, R., Ilkiv bx, I., Inaba dt, M., Incani w, E., Innocenti y, G. M., Ionita ah, C., Ippolitov ct, M., Irfan r, M., Ivanov cq, M., Ivanov cf, V., Ivanytskyi c, O., Jachołkowski aa, A., Jahnke dm, C., Jang bo, H. J., Janik dz, M. A., Jayarathna do, P. H. S. Y., Jena as, S., Jimenez Bustamante bj, R. T., Jones cv, P. G., Jung ao, H., Jusko cv, A., Kalcher an, S., Kalinak bf, P., Kalweit ah, A., Kamin ax, J., Kang ed, J. H., Kaplin bw, V., Kar dx, S., Karasu Uysal bp, A., Karavichev bc, O., Karavicheva bc, T., Karpechev bc, E., Kebschull aw, U., Keidel ee, R., Ketzer ai, B., Khan r, M. M., 3, Khan cu, P., Khan dx, S. A., Khanzadeev cf, A., Kharlov bb, Y., Kileng aj, B., Kim ed, B., Kim bo, D. W., Kim dp, D. J., Kim ao, J. S., Kim ao, M., Kim ed, M., Kim t, S., Kim ed, T., Kirsch an, S., Kisel an, I., Kiselev be, S., Kisiel dz, A., Kiss eb, G., Klay f, J. L., Klein cm, J., Klein Bösing az, C., Kluge ah, A., Knichel cq, M. L., Knospe dk, A. G., Kobdaj dg, C., Köhler cq, M. K., Kollegger an, T., Kolojvari dw, A., Kondratiev dw, V., Kondratyeva bw, N., Konevskikh bc, A., Kovalenko dw, V., Kowalski dj, M., Kox br, S., Koyithatta Meethaleveedu as, G., Kral dp, J., Králik bf, I., Kramer ax, F., Kravcˇáková am, A., Krelina al, M., Kretz an, M., Krivda cv, M., Krizek cd, F., Krus al, M., Kryshen cf, E., Krzewicki cq, M., Kucˇera cd, V., Kucheriaev ct, Y., Kugathasan ah, T., Kuhn ba, C., Kuijer cb, P. G., Kulakov ax, I., Kumar as, J., Kurashvili bx, P., Kurepin bc, A., Kurepin bc, A. B., Kuryakin cs, A., Kushpil cd, S., Kushpil cd, V., Kweon cm, M. J., Kwon ed, Y., Ladron de Guevara bj, P., Lagana Fernandes dm, C., Lakomov av, I., Langoy dy, R., Lara aw, C., Lardeux df, A., Lattuca y, A., La Pointe bd, S. L., La Rocca aa, P., Lee cv, G. R., Legrand ah, I., Lehnert ax, J., Lemmon cc, R. C., Lenhardt cq, M., Lenti cx, V., Leogrande bd, E., Leoncino y, M., León Monzón dl, I., Lévai eb, P., Li bq, S., G, Lien dy, J., Q, Lietava cv, R., Lindal u, S., Lindenstruth an, V., Lippmann cq, C., Lisa s, M. A., Ljunggren af, H. M., Lodato bd, D. F., Loenne q, P. I., Loggins ea, V. R., Loginov bw, V., Lohner cm, D., Loizides bu, C., Lopez bq, X., López Torres i, E., Lu cm, X. G., Luettig ax, P., Lunardon ab, M., Luo g, J., Luzzi ah, C., Gago cw, A. M., Jacobs bu, P. M., Ma ec, R., Maevskaya bc, A., Mager ah, M., Mahapatra bh, D. P., Maire cm, A., Malaev cf, M., Maldonado Cervantes bj, I., Malinina bm, L., 4, Mal’Kevich be, D., Malzacher cq, P., Mamonov cs, A., Manceau de, L., Manko ct, V., Manso bq, F., Manzari cx, V., Marchisone bq, M., Y, Mareš bg, J., Margotti cy, A., Marín cq, A., Markert ah, C., Marquard ax, M., Martashvili dr, I., Martin cq, N. A., Martinengo ah, P., Martínez b, M. I., Martínez García df, G., Martin Blanco df, J., Martynov c, Y., Mas df, A., Masciocchi cq, S., Masera y, M., Masoni cz, A., Massacrier df, L., Mastroserio ae, A., Matyja dj, A., Mayer dj, C., Mazer dr, J., Mazumder at, R., Mazzoni dc, M. A., Meddi v, F., Menchaca Rocha bk, A., Mercado Pérez cm, J., Meres ak, M., Miake dt, Y., Mikhaylov be, K., Milano ah, L., Milosevic u, J., 5, Mischke bd, A., Mishra at, A. N., Mis ́kowiec cq, D., Mitu bi, C. M., Mlynarz ea, J., Mohanty dx, B., Molnar ba, L., Montaño Zetina k, L., Montes j, E., Morando ab, M., Moreira De Godoy dm, D. A., Moretto ab, S., Morreale dp, A., Morsch ah, A., Muccifora bs, V., Mudnic dh, E., Muhuri dx, S., Mukherjee dx, M., Müller ah, H., Munhoz dm, M. G., Murray cj, S., Musa ah, L., Musinsky bf, J., Nandi as, B. K., Nania cy, R., Nappi cx, E., Nattrass dr, C., Nayak dx, T. K., Nazarenko cs, S., Nedosekin be, A., Nicassio cq, M., Niculescu ah, M., Nielsen ca, B. S., Nikolaev ct, S., Nikulin ct, S., Nikulin cf, V., Nilsen cg, B. S., Noferini l, F., Nomokonov bm, P., Nooren bd, G., Nyanin ct, A., Nyatha as, A., Nystrand q, J., Oeschler cm, H., Oh ec, S., Oh bn, S. K., Ao, 6, Okatan bp, A., Olah eb, L., Oleniacz dz, J., Oliveira Da Silva dm, A. C., Onderwaater cq, J., Oppedisano de, C., Ortiz Velasquez af, A., Oskarsson af, A., Otwinowski cq, J., Oyama cm, K., Pachmayer cm, Y., Pachr al, M., Pagano ac, P., Paic ́ bj, G., Painke an, F., Pajares p, C., Pal dx, S. K., Palmeri da, A., Pant as, D., Papikyan a, V., Pappalardo da, G. S., Park cq, W. J., Passfeld az, A., Patalakha bb, D. I., Paticchio cx, V., Paul cu, B., Pawlak dz, T., Peitzmann bd, T., Pereira Da Costa n, H., Pereira De Oliveira Filho dm, E., Peresunko ct, D., Pérez Lara cb, C. E., Peryt dz, W., Pesci cy, A., Pestov e, Y., Petrácˇek al, V., Petran al, M., Petris by, M., Petrovici by, M., Petta aa, C., Pikna ak, M., Pillot df, P., Pinazza ah, O., Pinsky do, L., Piyarathna do, D. B., Planinic cr, M., Płoskon ́ bu, M., Pluta dz, J., Pochybova eb, S., Podesta Lerma dl, P. L. M., Poghosyan ah, M. G., Pohjoisaho aq, E. H. O., Polichtchouk bb, B., Poljak cr, N., Pop by, A., Porteboeuf Houssais bq, S., Porter bu, J., Pospisil al, V., Potukuchi ck, B., Prasad ea, S. K., D, Preghenella cy, R., Prino de, F., Pruneau ea, C. A., Pshenichnov bc, I., Puddu w, G., Pujahari ea, P., Punin cs, V., Putschke ea, J., Qvigstad u, H., Rachevski dd, A., Raha d, S., Rak dp, J., Rakotozafindrabe n, A., Ramello ad, L., Raniwala cl, R., Raniwala cl, S., Räsänen aq, S. S., Rascanu ax, B. T., Rathee ch, D., Rauf o, A. W., Razazi w, V., Read dr, K. F., Real br, J. S., Redlich bx, K., 7, Reed ec, R. J., Rehman q, A., Reichelt ax, P., Reicher bd, M., Reidt ah, F., Renfordt ax, R., Reolon bs, A. R., Reshetin bc, A., Rettig an, F., Revol ah, J. P., Reygers cm, K., Riabov cf, V., Ricci bt, R. A., Richert af, T., Richter u, M., Riedler ah, P., Riegler ah, W., Riggi aa, F., Rivetti de, A., Rocco bd, E., Rodríguez Cahuantzi b, M., Rodriguez Manso cb, A., Røed u, K., Rogochaya bm, E., Rohni ck, S., Rohr an, D., Röhrich q, D., Romita dq, R., Ronchetti bs, F., Ronflette df, L., Rosnet bq, P., Rossegger ah, S., Rossi ah, A., Roy at, A., Roy ba, C., Roy cu, P., Rubio Montero j, A. J., Russo y, R., Ryabinkin ct, E., Ryabov cf, Y., Rybicki dj, A., Sadovsky bb, S., Šafarˇík ah, K., Sahlmuller ax, B., Sahoo at, R., Sahu bh, P. K., Saini dx, J., Salgado p, C. A., Salzwedel s, J., Sambyal ck, S., Samsonov cf, V., Sanchez Castro ba, X., Sánchez Rodríguez dl, F. J., Šándor bf, L., Sandoval bk, A., Sano dt, M., Santagati aa, G., Sarkar dx, D., Scapparone cy, E., Scarlassara ab, F., Scharenberg co, R. P., Schiaua by, C., Schicker cm, R., Schmidt cq, C., Schmidt ag, H. R., Schuchmann ax, S., Schukraft ah, J., Schulc al, M., Schuster ec, T., Schutz ah, Y., Schwarz cq, K., Schweda cq, K., Scioli z, G., Scomparin de, E., Scott cv, P. A., Scott dr, R., Segato ab, G., Seger cg, J. E., Selyuzhenkov cq, I., Seo cp, J., Serradilla j, E., Sevcenco bi, A., Shabetai df, A., Shabratova bm, G., Shahoyan ah, R., Shangaraev bb, A., Sharma dr, N., Sharma ck, S., Shigaki ar, K., Shtejer y, K., Sibiriak ct, Y., Siddhanta cz, S., Siemiarczuk bx, T., Silvermyr ce, D., Silvestre br, C., Simatovic du, G., Singaraju dx, R., Singh ck, R., Singha bz, S., Singhal dx, V., Sinha dx, B. C., Sinha cu, T., Sitar ak, B., Sitta ad, M., Skaali u, T. B., Skjerdal q, K., Smakal al, R., Smirnov ec, N., Snellings bd, R. J. M., Søgaard af, C., Soltz bv, R., Song cp, J., Song ed, M., Soramel ab, F., Sorensen dr, S., Spacek al, M., Sputowska dj, I., Spyropoulou Stassinaki ci, M., Srivastava co, B. K., Stachel cm, J., Stan bi, I., Stefanek bx, G., Steinpreis s, M., Stenlund af, E., Steyn bl, G., Stiller cm, J. H., Stocco df, D., Stolpovskiy bb, M., Strmen ak, P., Suaide dm, A. A. P., Subieta Vasquez y, M. A., Sugitate ar, T., Suire av, C., Suleymanov o, M., Sultanov be, R., Šumbera cd, M., Susa cr, T., Symons bu, T. J. M., Szanto de Toledo dm, A., Szarka ak, I., Szczepankiewicz ah, A., Szymanski dz, M., Takahashi dn, J., Tangaro ae, M. A., Tapia Takaki av, J. D., 8, Tarantola Peloni ax, A., Tarazona Martinez ah, A., Tauro ah, A., Tejeda Muñoz b, G., Telesca ah, A., Terrevoli ae, C., Ter Minasyan ct, A., Thäder cq, J., Thomas bd, D., Tieulent dv, R., Timmins do, A. R., Toia db, A., Torii ds, H., Trubnikov c, V., Trzaska dp, W. H., Tsuji ds, T., Tumkin cs, A., Turrisi db, R., Tveter u, T. S., Ulery ax, J., Ullaland q, K., Ulrich aw, J., Uras dv, A., Usai w, G. L., Vajzer cd, M., Vala bf, M., Valencia Palomo bq, L., Vallero y, S., Vande Vyvre ah, P., Vannucci bt, L., Van Hoorne ah, J. W., van Leeuwen bd, M., Vargas b, A., Varma as, R., Vasileiou ci, M., Vasiliev ct, A., Vechernin dw, V., Veldhoen bd, M., Venaruzzo x, M., Vercellin y, E., Vergara Limón b, S., Vernet h, R., Verweij ea, M., Vickovic dh, L., Viesti ab, G., Viinikainen dp, J., Vilakazi bl, Z., Villalobos Baillie cv, O., Vinogradov ct, A., Vinogradov dw, L., Vinogradov cs, Y., Virgili ac, T., Viyogi dx, Y. P., Vodopyanov bm, A., Völkl cm, M. A., Voloshin be, K., Voloshin ea, S. A., Volpe ah, G., von Haller ah, B., Vorobyev dw, I., Vranic cq, D., Vrláková am, J., Vulpescu bq, B., Vyushin cs, A., Wagner q, B., Wagner cq, J., Wagner al, V., Wang g, M., Wang cm, Y., Watanabe dt, D., Weber do, M., Wessels az, J. P., Westerhoff az, U., Wiechula ag, J., Wikne u, J., Wilde az, M., Wilk bx, G., Wilkinson cm, J., Williams cy, M. C. S., Windelband cm, B., Winn cm, M., Xiang g, C., Yaldo ea, C. G., Yamaguchi ds, Y., Yang n, H., Yang g, P., Yang q, S., Yano ar, S., Yasnopolskiy ct, S., Yi cp, J., Yin g, Z., Yoo cp, I. K., Yushmanov ct, I., Zaccolo ca, V., Zach al, C., Zaman o, A., Zampolli cy, C., Zaporozhets bm, S., Zarochentsev dw, A., Závada bg, P., Zaviyalov cs, N., Zbroszczyk dz, H., Zgura bi, I. S., Zhalov cf, M., Zhang g, F., Zhang g, H., Zhang bq, X., Bu, G, Zhang g, Y., Zhao u, C., Zhou g, D., Zhou g, F., Zhou bd, Y., Zhu g, H., Zhu g, J., Zhu g, X., Zichichi l, A., Zimmermann cm, A., Zimmermann ah, M. B., Zinovjev c, G., Zoccarato dv, Y., Zynovyev c, M., Zyzak, M., Contin, Giacomo, Piano, Stefano, Lea, Ramona, Camerini, Paolo, Luparello, Grazia, Fragiacomo, Enrico, Margagliotti, Giacomo, Rui, Rinaldo, B., Abelev bv, J., Adam al, D., Adamová cd, M. M., Aggarwal ch, G., Aglieri Rinella ah, M., Agnello cn, De, A. G., Agocs eb, A., Agostinelli z, N., Agrawal a, Z., Ahammed dx, N., Ahmad r, A., Ahmad Masoodi r, I., Ahmed o, S. U., Ahn bo, S. A., Ahn bo, I., Aimo de, Cn, S., Aiola ec, M., Ajaz o, A., Akindinov be, D., Aleksandrov ct, B., Alessandro de, D., Alexandre cv, A., Alici l, Cy, A., Alkin c, J., Alme aj, T., Alt an, V., Altini ae, S., Altinpinar q, I., Altsybeev dw, C., Alves Garcia Prado dm, C., Andrei by, A., Andronic cq, V., Anguelov cm, J., Anielski az, T., Anticˇic ́ cr, F., Antinori db, P., Antonioli cy, L., Aphecetche df, H., Appelshäuser ax, N., Arbor br, S., Arcelli z, N., Armesto p, R., Arnaldi de, T., Aronsson ec, I. C., Arsene u, Cq, M., Arslandok ax, A., Augustinus ah, R., Averbeck cq, T. C., Awes ce, M. D., Azmi r, Cj, M., Bach an, A., Badalà da, Y. W., Baek ao, Bq, S., Bagnasco de, R., Bailhache ax, V., Bairathi cl, R., Bala ck, A., Baldisseri n, F., Baltasar Dos Santos Pedrosa ah, J., Bán bf, R. C., Baral bh, R., Barbera aa, F., Barile ae, G. G., Barnaföldi eb, L. S., Barnby cv, V., Barret bq, J., Bartke dj, M., Basile z, N., Bastid bq, S., Basu dx, B., Bathen az, G., Batigne df, B., Batyunya bm, P. C., Batzing u, C., Baumann ax, I. G., Bearden ca, H., Beck ax, C., Bedda cn, N. K., Behera a, I., Belikov ba, F., Bellini z, R., Bellwied do, E., Belmont Moreno bk, G., Bencedi eb, S., Beole y, I., Berceanu by, A., Bercuci by, Y., Berdnikov cf, D., Berenyi eb, M. E., Berger di, A. A. E., Bergognon df, R. A., Bertens bd, D., Berzano y, L., Betev ah, A., Bhasin ck, A. K., Bhati ch, B., Bhattacharjee ap, J., Bhom dt, L., Bianchi y, N., Bianchi b, C., Bianchin bd, J., Bielcˇík al, J., Bielcˇíková cd, A., Bilandzic ca, S., Bjelogrlic bd, F., Blanco j, D., Blau ct, C., Blume ax, F., Bock bu, Cm, F. V., Boehmer di, A., Bogdanov bw, H., Bøggild ca, M., Bogolyubsky bb, L., Boldizsár eb, M., Bombara am, J., Book ax, H., Borel n, A., Borissov cp, Ea, J., Bornschein an, F., Bossú bl, M., Botje cb, E., Botta y, S., Böttger aw, P., Braun Munzinger cq, M., Bregant dm, Df, T., Breitner aw, T. A., Broker ax, T. A., Browning co, M., Broz ak, E., Bruna de, G. E., Bruno ae, D., Budnikov c, H., Buesching ax, S., Bufalino de, P., Buncic ah, O., Busch cm, Z., Buthelezi bl, D., Caffarri ab, X., Cai g, H., Caines ec, A., Caliva bd, E., Calvo Villar cw, V., Canoa Roman ah, F., Carena ah, W., Carena ah, F., Carminati ah, A., Casanova Díaz b, J., Castillo Castellanos n, E. A. R., Casula w, V., Catanescu by, C., Cavicchioli ah, C., Ceballos Sanchez i, J., Cepila al, P., Cerello de, B., Chang dp, S., Chapeland ah, J. L., Charvet n, S., Chattopadhyay dx, S., Chattopadhyay cu, M., Cherney cg, C., Cheshkov dv, B., Cheynis dv, V., Chibante Barroso ah, D. D., Chinellato do, Dn, P., Chochula ah, M., Chojnacki ca, S., Choudhury dx, P., Christakoglou cb, C. H., Christensen ca, P., Christiansen af, T., Chujo dt, S. U., Chung cp, C., Cicalo cz, L., Cifarelli l, Z, F., Cindolo cy, J., Cleymans cj, F., Colamaria ae, D., Colella ae, A., Collu w, M., Colocci z, G., Conesa Balbastre br, Z., Conesa del Valle av, Ah, M. E., Connors ec, G., Contin x, J. G., Contreras k, T. M., Cormier ce, Y., Corrales Morales y, P., Cortese ad, I., Cortés Maldonado b, M. R., Cosentino bu, Dm, F., Costa ah, P., Crochet bq, R., Cruz Albino k, E., Cuautle bj, L., Cunqueiro b, A., Dainese db, R., Dang g, A., Danu bi, D., Das cu, I., Das av, K., Das cu, S., Das d, A., Dash dn, S., Dash a, S., De dx, H., Delagrange df, A., Deloff bx, E., Dénes eb, G., D’Erasmo ae, G. O. V., de Barros dm, A., De Caro l, Ac, G., de Cataldo cx, J., de Cuveland an, A., De Falco w, D., De Gruttola ac, L, N., De Marco de, S., De Pasquale ac, R., de Rooij bd, M. A., Diaz Corchero j, T., Dietel az, R., Divià ah, D., Di Bari ae, S., Di Liberto dc, A., Di Mauro ah, P., Di Nezza b, Ø., Djuvsland q, A., Dobrin bd, T., Dobrowolski bx, D., Domenicis Gimenez dm, B., Dönigus ax, O., Dordic u, S., Dorheim di, A. K., Dubey dx, A., Dubla bd, L., Ducroux dv, P., Dupieux bq, A. K., Dutta Majumdar cu, D., Elia cx, H., Engel aw, B., Erazmus ah, H. A., Erdal aj, D., Eschweiler an, B., Espagnon av, M., Estienne df, S., Esumi dt, D., Evans cv, S., Evdokimov bb, G., Eyyubova u, D., Fabris db, J., Faivre br, D., Falchieri z, A., Fantoni b, M., Fasel cm, D., Fehlker q, L., Feldkamp az, D., Felea bi, A., Feliciello de, G., Feofilov dw, J., Ferencei cd, A., Fernández Téllez b, E. G., Ferreiro p, A., Ferretti y, A., Festanti ab, J., Figiel dj, M. A. S., Figueredo dm, Dq, S., Filchagin c, D., Finogeev bc, F. M., Fionda ae, E. M., Fiore ae, E., Floratos ci, M., Floris ah, S., Foertsch bl, P., Foka cq, S., Fokin ct, A., Francescon ab, U., Frankenfeld cq, U., Fuchs ah, C., Furget br, M., Fusco Girard ac, J. J., Gaardhøje ca, M., Gagliardi y, M., Gallio y, D. R., Gangadharan, Bu, P., Ganoti ce, Ci, C., Garabatos cq, E., Garcia Solis m, C., Gargiulo ah, I., Garishvili bv, J., Gerhard an, M., Germain df, A., Gheata ah, M., Gheata ah, Bi, B., Ghidini ae, P., Ghosh dx, S. K., Ghosh d, P., Gianotti b, P., Giubellino ah, E., Gladysz Dziadus dj, P., Glässel cm, R., Gomez k, P., González Zamora j, S., Gorbunov an, L., Görlich dj, S., Gotovac dh, L. K., Graczykowski dz, R., Grajcarek cm, A., Grelli bd, A., Grigoras ah, C., Grigoras ah, V., Grigoriev bw, A., Grigoryan a, S., Grigoryan bm, B., Grinyov c, N., Grion dd, J. F., Grosse Oetringhaus ah, J. Y., Grossiord dv, R., Grosso ah, F., Guber bc, R., Guernane br, B., Guerzoni z, M., Guilbaud dv, K., Gulbrandsen ca, H., Gulkanyan a, T., Gunji d, A., Gupta ck, R., Gupta ck, K. H., Khan o, R., Haake az, Ø., Haaland q, C., Hadjidakis av, M., Haiduc bi, H., Hamagaki d, G., Hamar eb, L. D., Hanratty cv, A., Hansen ca, J. W., Harris ec, H., Hartmann an, A., Harton m, D., Hatzifotiadou cy, S., Hayashi d, A., Hayrapetyan ah, A, S. T., Heckel ax, M., Heide az, H., Helstrup aj, A., Herghelegiu by, G., Herrera Corral k, B. A., Hess ag, K. F., Hetland aj, B., Hicks ec, B., Hippolyte ba, J., Hladky bg, P., Hristov ah, M., Huang q, T. J., Humanic, D., Hutter an, D. S., Hwang t, J. C., Ianigro dv, R., Ilkaev c, I., Ilkiv bx, M., Inaba dt, E., Incani w, G. M., Innocenti y, C., Ionita ah, M., Ippolitov ct, M., Irfan r, M., Ivanov cq, V., Ivanov cf, O., Ivanytskyi c, A., Jachołkowski aa, C., Jahnke dm, H. J., Jang bo, M. A., Janik dz, P. H. S. Y., Jayarathna do, S., Jena a, Do, R. T., Jimenez Bustamante bj, P. G., Jones cv, H., Jung ao, A., Jusko cv, S., Kalcher an, P., Kalinak bf, A., Kalweit ah, J., Kamin ax, J. H., Kang ed, V., Kaplin bw, S., Kar dx, A., Karasu Uysal bp, O., Karavichev bc, T., Karavicheva bc, E., Karpechev bc, U., Kebschull aw, R., Keidel ee, B., Ketzer ai, Di, M. M., Khan r, P., Khan cu, S. A., Khan dx, A., Khanzadeev cf, Y., Kharlov bb, B., Kileng aj, B., Kim ed, D. W., Kim bo, Ao, D. J., Kim dp, J. S., Kim ao, M., Kim ao, M., Kim ed, S., Kim t, T., Kim ed, S., Kirsch an, I., Kisel an, S., Kiselev be, A., Kisiel dz, G., Kiss eb, J. L., Klay f, J., Klein cm, C., Klein Bösing az, A., Kluge ah, M. L., Knichel cq, A. G., Knospe dk, C., Kobdaj dg, M. K., Köhler cq, T., Kollegger an, A., Kolojvari dw, V., Kondratiev dw, N., Kondratyeva bw, A., Konevskikh bc, V., Kovalenko dw, M., Kowalski dj, S., Kox br, G., Koyithatta Meethaleveedu a, J., Kral dp, I., Králik bf, F., Kramer ax, A., Kravcˇáková am, M., Krelina al, M., Kretz an, M., Krivda cv, Bf, F., Krizek cd, Aq, M., Krus al, E., Kryshen cf, M., Krzewicki cq, V., Kucˇera cd, Y., Kucheriaev ct, T., Kugathasan ah, C., Kuhn ba, P. G., Kuijer cb, I., Kulakov ax, J., Kumar a, P., Kurashvili bx, A., Kurepin bc, A. B., Kurepin bc, A., Kuryakin c, S., Kushpil cd, V., Kushpil cd, M. J., Kweon cm, Au, Y., Kwon ed, P., Ladron de Guevara bj, C., Lagana Fernandes dm, I., Lakomov av, R., Langoy dy, C., Lara aw, A., Lardeux df, A., Lattuca y, S. L., La Pointe bd, P., La Rocca aa, G. R., Lee cv, I., Legrand ah, J., Lehnert ax, R. C., Lemmon cc, M., Lenhardt cq, V., Lenti cx, E., Leogrande bd, M., Leoncino y, I., León Monzón dl, P., Lévai eb, S., Li bq, G, J., Lien dy, Q, R., Lietava cv, S., Lindal u, V., Lindenstruth an, C., Lippmann cq, M. A., Lisa, H. M., Ljunggren af, D. F., Lodato bd, P. I., Loenne q, V. R., Loggins ea, V., Loginov bw, D., Lohner cm, C., Loizides bu, X., Lopez bq, E., López Torres i, X. G., Lu cm, P., Luettig ax, M., Lunardon ab, J., Luo g, C., Luzzi ah, A. M., Gago cw, P. M., Jacobs bu, R., Ma ec, A., Maevskaya bc, M., Mager ah, D. P., Mahapatra bh, A., Maire cm, Ba, M., Malaev cf, I., Maldonado Cervantes bj, L., Malinina bm, D., Mal’Kevich be, P., Malzacher cq, A., Mamonov c, L., Manceau de, V., Manko ct, F., Manso bq, V., Manzari cx, M., Marchisone bq, Y, J., Mareš bg, A., Margotti cy, A., Marín cq, C., Markert ah, Dk, M., Marquard ax, I., Martashvili dr, N. A., Martin cq, P., Martinengo ah, M. I., Martínez b, G., Martínez García df, J., Martin Blanco df, Y., Martynov c, A., Mas df, S., Masciocchi cq, M., Masera y, A., Masoni cz, L., Massacrier df, A., Mastroserio ae, A., Matyja dj, C., Mayer dj, J., Mazer dr, R., Mazumder at, M. A., Mazzoni dc, F., Meddi v, A., Menchaca Rocha bk, J., Mercado Pérez cm, M., Meres ak, Y., Miake dt, K., Mikhaylov be, Bm, L., Milano ah, J., Milosevic u, A., Mischke bd, A. N., Mishra at, D., Mis ́kowiec cq, C. M., Mitu bi, J., Mlynarz ea, B., Mohanty dx, Bz, L., Molnar ba, L., Montaño Zetina k, E., Montes j, M., Morando ab, D. A., Moreira De Godoy dm, S., Moretto ab, A., Morreale dp, A., Morsch ah, V., Muccifora b, E., Mudnic dh, S., Muhuri dx, M., Mukherjee dx, H., Müller ah, M. G., Munhoz dm, S., Murray cj, Bl, L., Musa ah, J., Musinsky bf, B. K., Nandi a, R., Nania cy, E., Nappi cx, C., Nattrass dr, T. K., Nayak dx, S., Nazarenko c, A., Nedosekin be, M., Nicassio cq, M., Niculescu ah, B. S., Nielsen ca, S., Nikolaev ct, S., Nikulin ct, V., Nikulin cf, B. S., Nilsen cg, F., Noferini l, P., Nomokonov bm, G., Nooren bd, A., Nyanin ct, A., Nyatha a, J., Nystrand q, H., Oeschler cm, Ay, S., Oh ec, S. K., Oh bn, Ao, 6, A., Okatan bp, L., Olah eb, J., Oleniacz dz, A. C., Oliveira Da Silva dm, J., Onderwaater cq, C., Oppedisano de, A., Ortiz Velasquez af, A., Oskarsson af, J., Otwinowski cq, K., Oyama cm, Y., Pachmayer cm, M., Pachr al, P., Pagano ac, G., Paic ́ bj, F., Painke an, C., Pajares p, S. K., Pal dx, A., Palmeri da, D., Pant a, V., Papikyan a, G. S., Pappalardo da, W. J., Park cq, A., Passfeld az, D. I., Patalakha bb, V., Paticchio cx, B., Paul cu, T., Pawlak dz, T., Peitzmann bd, H., Pereira Da Costa n, E., Pereira De Oliveira Filho dm, D., Peresunko ct, C. E., Pérez Lara cb, W., Peryt dz, A., Pesci cy, Y., Pestov e, V., Petrácˇek al, M., Petran al, M., Petris by, M., Petrovici by, C., Petta aa, M., Pikna ak, P., Pillot df, O., Pinazza ah, L., Pinsky do, D. B., Piyarathna do, M., Planinic cr, Du, M., Płoskon ́ bu, J., Pluta dz, S., Pochybova eb, P. L. M., Podesta Lerma dl, M. G., Poghosyan ah, Cg, E. H. O., Pohjoisaho aq, B., Polichtchouk bb, N., Poljak cr, A., Pop by, S., Porteboeuf Houssais bq, J., Porter bu, V., Pospisil al, B., Potukuchi ck, S. K., Prasad ea, D, R., Preghenella cy, F., Prino de, C. A., Pruneau ea, I., Pshenichnov bc, G., Puddu w, P., Pujahari ea, As, V., Punin c, J., Putschke ea, H., Qvigstad u, A., Rachevski dd, S., Raha d, J., Rak dp, A., Rakotozafindrabe n, L., Ramello ad, R., Raniwala cl, S., Raniwala cl, S. S., Räsänen aq, B. T., Rascanu ax, D., Rathee ch, A. W., Rauf o, V., Razazi w, K. F., Read dr, J. S., Real br, K., Redlich bx, R. J., Reed ec, A., Rehman q, P., Reichelt ax, M., Reicher bd, F., Reidt ah, R., Renfordt ax, A. R., Reolon b, A., Reshetin bc, F., Rettig an, J. P., Revol ah, K., Reygers cm, V., Riabov cf, R. A., Ricci bt, T., Richert af, M., Richter u, P., Riedler ah, W., Riegler ah, F., Riggi aa, A., Rivetti de, E., Rocco bd, M., Rodríguez Cahuantzi b, A., Rodriguez Manso cb, K., Røed u, E., Rogochaya bm, S., Rohni ck, D., Rohr an, D., Röhrich q, R., Romita dq, Cc, F., Ronchetti b, L., Ronflette df, P., Rosnet bq, S., Rossegger ah, A., Rossi ah, A., Roy at, C., Roy ba, P., Roy cu, A. J., Rubio Montero j, R., Russo y, E., Ryabinkin ct, Y., Ryabov cf, A., Rybicki dj, S., Sadovsky bb, K., Šafarˇík ah, B., Sahlmuller ax, R., Sahoo at, P. K., Sahu bh, J., Saini dx, C. A., Salgado p, J., Salzwedel, S., Sambyal ck, V., Samsonov cf, X., Sanchez Castro ba, Bj, F. J., Sánchez Rodríguez dl, L., Šándor bf, A., Sandoval bk, M., Sano dt, G., Santagati aa, D., Sarkar dx, E., Scapparone cy, F., Scarlassara ab, R. P., Scharenberg co, C., Schiaua by, R., Schicker cm, C., Schmidt cq, H. R., Schmidt ag, S., Schuchmann ax, J., Schukraft ah, M., Schulc al, T., Schuster ec, Y., Schutz ah, K., Schwarz cq, K., Schweda cq, G., Scioli z, E., Scomparin de, P. A., Scott cv, R., Scott dr, G., Segato ab, J. E., Seger cg, I., Selyuzhenkov cq, J., Seo cp, E., Serradilla j, Bk, A., Sevcenco bi, A., Shabetai df, G., Shabratova bm, R., Shahoyan ah, A., Shangaraev bb, N., Sharma dr, Bh, S., Sharma ck, K., Shigaki ar, K., Shtejer y, Y., Sibiriak ct, S., Siddhanta cz, T., Siemiarczuk bx, D., Silvermyr ce, C., Silvestre br, G., Simatovic du, R., Singaraju dx, R., Singh ck, S., Singha bz, Dx, V., Singhal dx, B. C., Sinha dx, T., Sinha cu, B., Sitar ak, M., Sitta ad, T. B., Skaali u, K., Skjerdal q, R., Smakal al, N., Smirnov ec, R. J. M., Snellings bd, C., Søgaard af, R., Soltz bv, J., Song cp, M., Song ed, F., Soramel ab, S., Sorensen dr, M., Spacek al, I., Sputowska dj, M., Spyropoulou Stassinaki ci, B. K., Srivastava co, J., Stachel cm, I., Stan bi, G., Stefanek bx, M., Steinpreis, E., Stenlund af, G., Steyn bl, J. H., Stiller cm, D., Stocco df, M., Stolpovskiy bb, P., Strmen ak, A. A. P., Suaide dm, M. A., Subieta Vasquez y, T., Sugitate ar, C., Suire av, M., Suleymanov o, R., Sultanov be, M., Šumbera cd, T., Susa cr, T. J. M., Symons bu, A., Szanto de Toledo dm, I., Szarka ak, A., Szczepankiewicz ah, M., Szymanski dz, J., Takahashi dn, M. A., Tangaro ae, J. D., Tapia Takaki av, A., Tarantola Peloni ax, A., Tarazona Martinez ah, A., Tauro ah, G., Tejeda Muñoz b, A., Telesca ah, C., Terrevoli ae, A., Ter Minasyan ct, Bw, J., Thäder cq, D., Thomas bd, R., Tieulent dv, A. R., Timmins do, A., Toia db, Ax, H., Torii d, V., Trubnikov c, W. H., Trzaska dp, T., Tsuji d, A., Tumkin c, R., Turrisi db, T. S., Tveter u, J., Ulery ax, K., Ullaland q, J., Ulrich aw, A., Uras dv, G. L., Usai w, M., Vajzer cd, M., Vala bf, L., Valencia Palomo bq, Av, S., Vallero y, P., Vande Vyvre ah, L., Vannucci bt, J. W., Van Hoorne ah, M., van Leeuwen bd, A., Vargas b, R., Varma a, M., Vasileiou ci, A., Vasiliev ct, V., Vechernin dw, M., Veldhoen bd, M., Venaruzzo x, E., Vercellin y, S., Vergara Limón b, R., Vernet h, M., Verweij ea, L., Vickovic dh, G., Viesti ab, J., Viinikainen dp, Z., Vilakazi bl, O., Villalobos Baillie cv, A., Vinogradov ct, L., Vinogradov dw, Y., Vinogradov c, T., Virgili ac, Y. P., Viyogi dx, A., Vodopyanov bm, M. A., Völkl cm, K., Voloshin be, S. A., Voloshin ea, G., Volpe ah, B., von Haller ah, I., Vorobyev dw, D., Vranic cq, J., Vrláková am, B., Vulpescu bq, A., Vyushin c, B., Wagner q, J., Wagner cq, V., Wagner al, M., Wang g, Y., Wang cm, D., Watanabe dt, M., Weber do, J. P., Wessels az, U., Westerhoff az, J., Wiechula ag, J., Wikne u, M., Wilde az, G., Wilk bx, J., Wilkinson cm, M. C. S., Williams cy, B., Windelband cm, M., Winn cm, C., Xiang g, C. G., Yaldo ea, Y., Yamaguchi d, H., Yang n, Bd, P., Yang g, S., Yang q, S., Yano ar, S., Yasnopolskiy ct, J., Yi cp, Z., Yin g, I. K., Yoo cp, I., Yushmanov ct, Zaccolo ca, V., C., Zach al, A., Zaman o, C., Zampolli cy, S., Zaporozhets bm, A., Zarochentsev dw, P., Závada bg, N., Zaviyalov c, H., Zbroszczyk dz, I. S., Zgura bi, M., Zhalov cf, F., Zhang g, H., Zhang g, X., Zhang bq, G, Bu, Y., Zhang g, C., Zhao u, D., Zhou g, F., Zhou g, Y., Zhou bd, H., Zhu g, J., Zhu g, X., Zhu g, A., Zichichi l, A., Zimmermann cm, M. B., Zimmermann ah, Az, G., Zinovjev c, Y., Zoccarato dv, M., Zynovyev c, M., Zyzak, and Contin, Giacomo

Subjects

Relativistic heavy ion collisions, Quarkonium, J/ψ suppression, Quark gluon plasma, Experimental results, Relativistic heavy ion collision

Abstract

The inclusive J/ψ nuclear modification factor (RAA) in Pb–Pb collisions at √sNN = 2.76 TeV has been measured by ALICE as a function of centrality in the e+e− decay channel at mid-rapidity (|y| < 0.8) and as a function of centrality, transverse momentum and rapidity in the μ+μ− decay channel at forward-rapidity (2.5 < y < 4). The J/ψ yields measured in Pb–Pb are suppressed compared to those in pp collisions scaled by the number of binary collisions. The RAA integrated over a centrality range corresponding to 90% of the inelastic Pb–Pb cross section is 0.72±0.06(stat.)±0.10(syst.) at mid-rapidity and 0.58 ± 0.01(stat.) ± 0.09(syst.) at forward-rapidity. At low transverse momentum, significantly larger values of RAA are measured at forward-rapidity compared to measurements at lower energy. These features suggest that a contribution to the J/ψ yield originates from charm quark (re)combination in the deconfined partonic medium.

Published

2014

3. High-dose therapy and peripheral blood progenitor cell transplantation: effects of recombinant human granulocyte-macrophage colony-stimulating factor on the autograft

Author

Bishop, MR, primary, Anderson, JR, additional, Jackson, JD, additional, Bierman, PJ, additional, Reed, EC, additional, Vose, JM, additional, Armitage, JO, additional, Warkentin, PI, additional, and Kessinger, A, additional

Published

1994

4. Allogeneic marrow transplantation in patients positive for hepatitis B surface antigen

Author

Reed, EC, primary, Myerson, D, additional, Corey, L, additional, and Meyers, JD, additional

Published

1991

5. Outcomes after hematopoietic stem-cell transplantation for hematologic malignancies in patients with or without advance care planning.

Author

Ganti AK, Lee SJ, Vose JM, Devetten MP, Bociek RG, Armitage JO, Bierman PJ, Maness LJ, Reed EC, and Loberiza FR Jr

Published

2007

6. INFORMAL DISCUSSION. THE RESERVOIRS ACT, 1975.

Author

COOLEY, P, ROBINSON, RD, REED, EC, JOHNSON, FG, and WHITE, SF

Published

1977

7. INFORMAL DISCUSSION. THE RESERVOIRS ACT, 1975.

Author

WHITE, SF, primary, REED, EC, additional, JOHNSON, FG, additional, COOLEY, P, additional, and ROBINSON, RD, additional

Published

1977

8. Internet Devices and Internet Access Among Migrant and Seasonal Farmworkers, North Carolina, 2023.

Author

Lee JGL, Roby M, Cofie LE, LePrevost CE, Harwell EL, Reed EC, Nieuwsma J, Bloss JE, Anderson GC, Santillán-Deras JR, Moore MA, Ketterman E, and Russell RG

Abstract

Objectives: Migrant and seasonal farmworkers work in rural areas where internet access may be limited. We assessed internet access, cost of access, and devices available to farmworkers through a statewide survey in North Carolina., Methods: During the 2023 agricultural season, we surveyed 1034 migrant and seasonal farmworkers during routine outreach visits in partnership with community health workers employed by 8 community health centers or by nonprofit health service agencies serving farmworkers in North Carolina. We surveyed participants aged ≥18 years by using time-venue sampling and surveyed up to 5 farmworkers at migrant housing locations. We weighted participants to the total population of farmworkers living in surveyed housing and calculated frequencies and percentages of internet access, internet speed, internet cost, available internet devices, and awareness and use of the Affordable Connectivity Program-a program that was run from 2021 through May 31, 2024, by the Federal Communications Commission to make internet access more affordable in the United States. We assessed predictors of internet access and ability to use online videos by using regression models., Results: Participants were predominantly Spanish-speaking men who lived in housing provided by farm owners. Among participants, 9.8% had internet connections with a cable or digital subscriber line, and 23.5% did not have consistent internet access. Most participants used cellular network internet (84.9%) and mobile phone devices (93.9%). Even among farmworkers who lived in their housing year-round, few had heard of (34.4%), applied to (4.8%), or used (2.0%) the Affordable Connectivity Program., Conclusions: Interventions are needed to increase internet access and digital inclusion for migrant and seasonal farmworkers in North Carolina. Development of state and county broadband infrastructure should consider farmworker housing., Competing Interests: Declaration of Conflicting InterestsThe authors declared no potential conflicts of interest with respect to the research, authorship, and/or publication of this article.

Published

2024

9. T H 17/Treg lymphocyte balance is regulated by beta adrenergic and cAMP signaling.

Author

Lauten TH, Elkhatib SK, Natour T, Reed EC, Jojo CN, and Case AJ

Abstract

Background: Post-traumatic stress disorder (PTSD) is a debilitating psychological disorder that also presents with neuroimmune irregularities. Patients display elevated sympathetic tone and are at an increased risk of developing secondary autoimmune diseases. Previously, using a mouse model of repeated social defeat stress (RSDS) that recapitulates certain features of PTSD, we demonstrated that elimination of sympathetic signaling to T-lymphocytes specifically limited their ability to produce pro-inflammatory interleukin 17A (IL-17A); a cytokine implicated in the development of many autoimmune disorders. However, the mechanism linking sympathetic signaling to T-lymphocyte IL-17A production remained unclear., Methods: Using a modified version of RSDS that allows for both males and females, as well as ex vivo models of T-lymphocyte polarization, we assessed the impact and mechanism of adrenergic receptor blockade (genetically and pharmacologically) and catecholamine depletion on T-lymphocyte differentiation to IL-17A-producing subtypes (i.e., T H 17)., Results: Only pharmacological inhibition of the beta 1 and 2 adrenergic receptors (β1/2) significantly decreased circulating IL-17A levels after RSDS, but did not impact other pro-inflammatory cytokines (e.g.,IL-6, TNF-α, and IL-10). This finding was confirmed using RSDS with both global β1/2 receptor knock-out mice, as well as by adoptively transferring β1/2 knock-out T-lymphocytes into immunodeficient hosts. Ex vivo polarized T-lymphocytes produced significantly less IL-17A with the blockade of β1/2 signaling, even in the absence of exogenous sympathetic neurotransmitter supplementation, which suggested T-lymphocyte-produced catecholamines may be involved in IL-17A production. Furthermore, cyclic AMP (cAMP) was demonstrated to be mechanistically involved in driving IL-17A production in T-lymphocytes, and amplifying cAMP signaling could restore IL-17A deficits caused by the absence of β1/2 signaling. Last, removal of β1/2 and cAMP signaling, even in IL-17A polarizing conditions, promoted regulatory T-lymphocyte (Treg) polarization, suggesting adrenergic signaling plays a role in the switching between pro- and anti-inflammatory T-lymphocyte subtypes., Conclusions: Our data depict a novel role for β1/2 adrenergic and cAMP signaling in the balance of T H 17/Treg lymphocytes. These findings provide a new target for pharmacological therapy in both psychiatric and autoimmune diseases associated with IL-17A-related pathology., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2024

10. Hemoglobin alpha is a redox-sensitive mitochondrial-related protein in T-lymphocytes.

Author

Reed EC, Silva VA, Giebel KR, Natour T, Lauten TH, Jojo CN, Schleiker AE, and Case AJ

Abstract

Hemoglobin subunits, which form the well-characterized, tetrameric, oxygen-carrying protein, have recently been described to be expressed in various non-canonical cell types. However, the exact function of hemoglobin subunits within these cells remains to be fully elucidated. Herein, we report for the first time, the expression of hemoglobin alpha-a1 (Hba-a1) in T-lymphocytes and describe its role as a mitochondrial-associated antioxidant. Within naïve T-lymphocytes, Hba-a1 mRNA and HBA protein are present and highly induced by redox perturbations, particularly those arising from the mitochondria. Additionally, preliminary data using a T-lymphocyte specific Hba-a1 knock-out mouse model indicated that the loss of Hba-a1 led to an exacerbated production of mitochondrial reactive oxygen species and inflammatory cytokines after a stress challenge, further supporting the role of HBA acting to buffer the mitochondrial redox environment. Interestingly, we observed Hba-a1 expression to be significantly upregulated or downregulated depending on T-lymphocyte polarization and metabolic state, which appeared to be controlled by both transcriptional regulation and chromatin remodeling. Altogether, these data suggest Hba-a1 may function as a crucial mitochondrial-associated antioxidant and appears to possess critical and complex functions related to T-lymphocyte activation and differentiation., Competing Interests: Conflict of Interest Statement: The authors have declared that no conflict of interest exists.

Published

2024

11. Electronic verification of identification cards for JUUL product purchase attempts after final consent judgement in North Carolina versus JUUL Labs, Inc. : evidence from Pitt County, North Carolina, 2022.

Author

Reed EC, Lee JGL, Hrywna M, Kong AY, Ackerman C, and Delnevo CD

Abstract

Competing Interests: Competing interests: AYK serves as a paid expert consultant in litigation against the tobacco industry. JGLL holds a royalty interest in tobacco retailer mapping system owned and licensed by the University of North Carolina at Chapel Hill. The software was not used in this research. All other authors report no competing interests.

Published

2024

12. Beta-adrenergic signaling and T-lymphocyte-produced catecholamines are necessary for interleukin 17A synthesis.

Author

Lauten TH, Elkhatib SK, Natour T, Reed EC, Jojo CN, and Case AJ

Abstract

Background: Post-traumatic stress disorder (PTSD) is a debilitating psychological disorder that also presents with neuroimmune irregularities. Patients display elevated sympathetic tone and are at an increased risk of developing secondary autoimmune diseases. Previously, using a preclinical model of PTSD, we demonstrated that elimination of sympathetic signaling to T-lymphocytes specifically limited their ability to produce pro-inflammatory interleukin 17A (IL-17A); a cytokine implicated in the development of many autoimmune disorders. However, the mechanism linking sympathetic signaling to T-lymphocyte IL-17A production remained unclear., Methods: Using a modified version of repeated social defeat stress (RSDS) that allows for both males and females, we assessed the impact of adrenergic receptor blockade (genetically and pharmacologically) and catecholamine depletion on T-lymphocyte IL-17A generation. Additionally, we explored the impact of adrenergic signaling and T-lymphocyte-produced catecholamines on both CD4+ and CD8+ T-lymphocytes polarized to IL-17A-producing phenotypes ex vivo., Results: Only pharmacological inhibition of the beta 1 and 2 adrenergic receptors (β1/2) significantly decreased circulating IL-17A levels after RSDS, but did not impact other pro-inflammatory cytokines (e.g., IL-6, TNF-α, and IL-10). This finding was confirmed using RSDS with both global β1/2 receptor knock-out mice, as well as by adoptively transferring β1/2 knock-out T-lymphocytes into immunodeficient hosts. Furthermore, ex vivo polarized T-lymphocytes produced significantly less IL-17A with the blockade of β1/2 signaling, even in the absence of exogenous sympathetic neurotransmitter supplementation, which suggested T-lymphocyte-produced catecholamines may be involved in IL-17A production. Indeed, pharmacological depletion of catecholamines both in vivo and ex vivo abrogated T-lymphocyte IL-17A production demonstrating the importance of immune-generated neurotransmission in pro-inflammatory cytokine generation., Conclusions: Our data depict a novel role for β1/2 adrenergic receptors and autologous catecholamine signaling during T-lymphocyte IL-17A production. These findings provide a new target for pharmacological therapy in both psychiatric and autoimmune diseases associated with IL-17A-related pathology., Competing Interests: Conflict of Interest The authors declare no competing financial interests in relation to the work described.

Published

2024

13. Repeated social defeat stress leads to immunometabolic shifts in innate immune cells of the spleen.

Author

Bekhbat M, Drake J, Reed EC, Lauten TH, Natour T, Vladimirov VI, and Case AJ

Abstract

Psychosocial stress has been shown to prime peripheral innate immune cells, which take on hyper-inflammatory phenotypes and are implicated in depressive-like behavior in mouse models. However, the impact of stress on cellular metabolic states that are thought to fuel inflammatory phenotypes in immune cells are unknown. Using single cell RNA-sequencing, we investigated mRNA enrichment of immunometabolic pathways in innate immune cells of the spleen in mice subjected to repeated social defeat stress (RSDS) or no stress (NS). RSDS mice displayed a significant increase in the number of splenic macrophages and granulocytes (p < 0.05) compared to NS littermates. RSDS-upregulated genes in macrophages, monocytes, and granulocytes significantly enriched immunometabolic pathways thought to play a role in myeloid-driven inflammation (glycolysis, HIF-1 signaling, MTORC1 signaling) as well as pathways related to oxidative phosphorylation (OXPHOS) and oxidative stress (p < 0.05 and FDR<0.1). These results suggest that the metabolic enhancement reflected by upregulation of glycolytic and OXPHOS pathways may be important for cellular proliferation of splenic macrophages and granulocytes following repeated stress exposure. A better understanding of these intracellular metabolic mechanisms may ultimately help develop novel strategies to reverse the impact of stress and associated peripheral immune changes on the brain and behavior., Competing Interests: None, (© 2023 Published by Elsevier Inc.)

Published

2023

14. Defining the nuanced nature of redox biology in post-traumatic stress disorder.

Author

Reed EC and Case AJ

Abstract

Post-traumatic stress disorder (PTSD) is a mental health disorder that arises after experiencing or witnessing a traumatic event. Despite affecting around 7% of the population, there are currently no definitive biological signatures or biomarkers used in the diagnosis of PTSD. Thus, the search for clinically relevant and reproducible biomarkers has been a major focus of the field. With significant advances of large-scale multi-omic studies that include genomic, proteomic, and metabolomic data, promising findings have been made, but the field still has fallen short. Amongst the possible biomarkers examined, one area is often overlooked, understudied, or inappropriately investigated: the field of redox biology. Redox molecules are free radical and/or reactive species that are generated as a consequence of the necessity of electron movement for life. These reactive molecules, too, are essential for life, but in excess are denoted as "oxidative stress" and often associated with many diseases. The few studies that have examined redox biology parameters have often utilized outdated and nonspecific methods, as well as have reported confounding results, which has made it difficult to conclude the role for redox in PTSD. Herein, we provide a foundation of how redox biology may underlie diseases like PTSD, critically examine redox studies of PTSD, and provide future directions the field can implement to enhance standardization, reproducibility, and accuracy of redox assessments for the use of diagnosis, prognosis, and therapy of this debilitating mental health disorder., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Reed and Case.)

Published

2023

15. S100a9 Protects Against the Effects of Repeated Social Defeat Stress.

Author

Moshfegh CM, Elkhatib SK, Watson GF, Drake J, Taylor ZN, Reed EC, Lauten TH, Clopp AJ, Vladimirov VI, and Case AJ

Abstract

Background: Posttraumatic stress disorder, a consequence of psychological trauma, is associated with increased inflammation and an elevated risk of developing comorbid inflammatory diseases. However, the mechanistic link between this mental health disorder and inflammation remains elusive. We previously found that S100a8 and S100a9 messenger RNA, genes that encode the protein calprotectin, were significantly upregulated in T lymphocytes and positively correlated with inflammatory gene expression and the mitochondrial redox environment in these cells. Therefore, we hypothesized that genetic deletion of calprotectin would attenuate the inflammatory and redox phenotype displayed after psychological trauma., Methods: We used a preclinical mouse model of posttraumatic stress disorder known as repeated social defeat stress (RSDS) combined with pharmacological and genetic manipulation of S100a9 (which functionally eliminates calprotectin). A total of 186 animals (93 control, 93 RSDS) were used in these studies., Results: Unexpectedly, we observed worsening of behavioral pathology, inflammation, and the mitochondrial redox environment in mice after RSDS compared with wild-type animals. Furthermore, loss of calprotectin significantly enhanced the metabolic demand on T lymphocytes, suggesting that this protein may play an undescribed role in mitochondrial regulation. This was further supported by single-cell RNA sequencing analysis demonstrating that RSDS and loss of S100a9 primarily altered genes associated with mitochondrial function and oxidative phosphorylation., Conclusions: These data demonstrate that the loss of calprotectin potentiates the RSDS-induced phenotype, which suggests that its observed upregulation after psychological trauma may provide previously unexplored protective functions., (© 2022 The Authors.)

Published

2022

16. The Relationship Between Perceived Confidence, Gender, and Writing in a Biomedical Engineering Research Experience for Undergraduates Site.

Author

Reed EC, Kain D, and George SM

Subjects

Female, Humans, Male, Students, Technology, Writing, Biomedical Engineering, Engineering

Abstract

Women frequently feel alienated in science, technology, engineering, and mathematics (STEM) environments due to gender biases, ultimately leading them to feel less competent or leave the field altogether. This study utilizes personal statements from a subset of participants from a National Science Foundation (NSF) funded Research Experiences for Undergraduates (REU) Site: Biomedical Engineering in Simulations, Imaging, and Modeling (BME-SIM) to investigate how confidence is shown by participants and how confidence is perceived by faculty reviewers in personal statements. This study compares feedback from faculty reviewers to perceived and self-reported confidence using lexical (i.e., word choices and use) and syntactic (i.e., structures of language segments such as sentences, phrases, and organization of words) features of these personal statements. Women received more negative feedback related to confidence compared to their male counterparts, notably in relation to modesty. Few differences were found between writing styles of genders in their pre- and post-program statements. Overall, writing styles did not seem to correlate with the genders' perceived or self-reported confidence; however, perception of confidence suggested a relationship between genders' pre- and post-program statements when examined by noun and adjective variation. A similar relationship was found between self-reported confidence and noun variation in men and women participants. Findings suggest that writing style perceptions and practices may be influenced by gender norms; however, without looking at the specific diction and content of personal statements, these conclusions cannot be fully established., (Copyright © 2021 by ASME.)

Published

2021

17. Dipole-phonon quantum logic with alkaline-earth monoxide and monosulfide cations.

Author

Mills M, Wu H, Reed EC, Qi L, Brown KR, Schneider C, Heaven MC, Campbell WC, and Hudson ER

Abstract

Dipole-phonon quantum logic (DPQL) leverages the interaction between polar molecular ions and the motional modes of a trapped-ion Coulomb crystal to provide a potentially scalable route to quantum information science. Here, we study a class of candidate molecular ions for DPQL, the cationic alkaline-earth monoxides and monosulfides, which possess suitable structure for DPQL and can be produced in existing atomic ion experiments with little additional complexity. We present calculations of DPQL operations for one of these molecules, CaO + , and discuss progress towards experimental realization. We also further develop the theory of DPQL to include state preparation and measurement and entanglement of multiple molecular ions.

Published

2020

18. NCCN Guidelines Insights: Breast Cancer, Version 3.2018.

Author

Goetz MP, Gradishar WJ, Anderson BO, Abraham J, Aft R, Allison KH, Blair SL, Burstein HJ, Dang C, Elias AD, Farrar WB, Giordano SH, Goldstein LJ, Isakoff SJ, Lyons J, Marcom PK, Mayer IA, Moran MS, Mortimer J, O'Regan RM, Patel SA, Pierce LJ, Reed EC, Rugo HS, Sitapati A, Smith KL, Smith ML, Soliman H, Telli ML, Ward JH, Young JS, Shead DA, and Kumar R

Subjects

Breast Neoplasms etiology, Female, Humans, Breast Neoplasms diagnosis, Breast Neoplasms therapy

Abstract

These NCCN Guidelines Insights highlight the updated recommendations for use of multigene assays to guide decisions on adjuvant systemic chemotherapy therapy for women with hormone receptor-positive, HER2-negative early-stage invasive breast cancer. This report summarizes these updates and discusses the rationale behind them., (Copyright © 2019 by the National Comprehensive Cancer Network.)

Published

2019

19. Breast Cancer, Version 4.2017, NCCN Clinical Practice Guidelines in Oncology.

Author

Gradishar WJ, Anderson BO, Balassanian R, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goetz MP, Goldstein LJ, Isakoff SJ, Lyons J, Marcom PK, Mayer IA, McCormick B, Moran MS, O'Regan RM, Patel SA, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Sitapati A, Smith KL, Smith ML, Soliman H, Somlo G, Telli ML, Ward JH, Kumar R, and Shead DA

Subjects

Breast Neoplasms etiology, Carcinoma, Ductal, Breast diagnosis, Carcinoma, Ductal, Breast etiology, Carcinoma, Ductal, Breast therapy, Carcinoma, Intraductal, Noninfiltrating diagnosis, Carcinoma, Intraductal, Noninfiltrating etiology, Carcinoma, Intraductal, Noninfiltrating therapy, Combined Modality Therapy, Disease Management, Female, Humans, Retreatment, Treatment Outcome, Watchful Waiting, Breast Neoplasms diagnosis, Breast Neoplasms therapy

Abstract

Ductal carcinoma in situ (DCIS) of the breast represents a heterogeneous group of neoplastic lesions in the breast ducts. The goal for management of DCIS is to prevent the development of invasive breast cancer. This manuscript focuses on the NCCN Guidelines Panel recommendations for the workup, primary treatment, risk reduction strategies, and surveillance specific to DCIS., (Copyright © 2018 by the National Comprehensive Cancer Network.)

Published

2018

20. NCCN Guidelines Insights: Breast Cancer, Version 1.2017.

Author

Gradishar WJ, Anderson BO, Balassanian R, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goetz MP, Goldstein LJ, Isakoff SJ, Lyons J, Marcom PK, Mayer IA, McCormick B, Moran MS, O'Regan RM, Patel SA, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Sitapati A, Smith KL, Smith ML, Soliman H, Somlo G, Telli M, Ward JH, Shead DA, and Kumar R

Subjects

Axilla, Combined Modality Therapy methods, Disease Management, Female, Humans, Neoplasm Staging, Sentinel Lymph Node Biopsy, Breast Neoplasms diagnosis, Breast Neoplasms therapy

Abstract

These NCCN Guidelines Insights highlight the important updates/changes to the surgical axillary staging, radiation therapy, and systemic therapy recommendations for hormone receptor-positive disease in the 1.2017 version of the NCCN Guidelines for Breast Cancer. This report summarizes these updates and discusses the rationale behind them. Updates on new drug approvals, not available at press time, can be found in the most recent version of these guidelines at NCCN.org., (Copyright © 2017 by the National Comprehensive Cancer Network.)

Published

2017

21. Invasive Breast Cancer Version 1.2016, NCCN Clinical Practice Guidelines in Oncology.

Author

Gradishar WJ, Anderson BO, Balassanian R, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goetz M, Goldstein LJ, Hudis CA, Isakoff SJ, Marcom PK, Mayer IA, McCormick B, Moran M, Patel SA, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Smith KL, Smith ML, Soliman H, Somlo G, Telli M, Ward JH, Shead DA, and Kumar R

Subjects

Chemotherapy, Adjuvant adverse effects, Combined Modality Therapy, Female, Fertility drug effects, Fertility Preservation, Humans, Mammaplasty methods, Mastectomy methods, Neoplasm Invasiveness, Neoplasm Staging, Radiotherapy, Adjuvant adverse effects, United States, Breast Neoplasms pathology, Breast Neoplasms therapy

Abstract

Breast cancer is the most common malignancy in women in the United States and is second only to lung cancer as a cause of cancer death. The overall management of breast cancer includes the treatment of local disease with surgery, radiation therapy, or both, and the treatment of systemic disease with cytotoxic chemotherapy, endocrine therapy, biologic therapy, or combinations of these. This article outlines the NCCN Guidelines specific to breast cancer that is locoregional (restricted to one region of the body), and discusses the management of clinical stage I, II, and IIIA (T3N1M0) tumors. For NCCN Guidelines on systemic adjuvant therapy after locoregional management of clinical stage I, II and IIIA (T3N1M0) and for management for other clinical stages of breast cancer, see the complete version of these guidelines at NCCN.org., (Copyright © 2016 by the National Comprehensive Cancer Network.)

Published

2016

22. NCCN Guidelines Insights Breast Cancer, Version 1.2016.

Author

Gradishar WJ, Anderson BO, Balassanian R, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goetz M, Goldstein LJ, Hudis CA, Isakoff SJ, Marcom PK, Mayer IA, McCormick B, Moran M, Patel SA, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Smith KL, Smith ML, Soliman H, Somlo G, Telli M, Ward JH, Shead DA, and Kumar R

Subjects

Female, Humans, Breast Neoplasms therapy

Abstract

These NCCN Guideline Insights highlight the important updates to the systemic therapy recommendations in the 2016 NCCN Guidelines for Breast Cancer. In the most recent version of these guidelines, the NCCN Breast Cancer Panel included a new section on the principles of preoperative systemic therapy. In addition, based on new evidence, the panel updated systemic therapy recommendations for women with hormone receptor-positive breast cancer in the adjuvant and metastatic disease settings and for patients with HER2-positive metastatic breast cancer. This report summarizes these recent updates and discusses the rationale behind them., (Copyright © 2015 by the National Comprehensive Cancer Network.)

Published

2015

23. Breast Cancer Version 2.2015.

Author

Gradishar WJ, Anderson BO, Balassanian R, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goetz M, Goldstein LJ, Hudis CA, Isakoff SJ, Marcom PK, Mayer IA, McCormick B, Moran M, Patel SA, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Smith KL, Smith ML, Soliman H, Somlo G, Telli M, Ward JH, Shead DA, and Kumar R

Subjects

Axilla, Breast Neoplasms diagnosis, Female, Humans, Mammaplasty, Neoplasm Staging, Radiotherapy, Breast Neoplasms pathology, Breast Neoplasms therapy, Lymph Node Excision, Mastectomy methods

Abstract

Breast cancer is the most common malignancy in women in the United States and is second only to lung cancer as a cause of cancer death. The overall management of breast cancer includes the treatment of local disease with surgery, radiation therapy, or both, and the treatment of systemic disease with cytotoxic chemotherapy, endocrine therapy, biologic therapy, or combinations of these. This portion of the NCCN Guidelines discusses recommendations specific to the locoregional management of clinical stage I, II, and IIIA (T3N1M0) tumors., (Copyright © 2015 by the National Comprehensive Cancer Network.)

Published

2015

24. Breast cancer version 3.2014.

Author

Gradishar WJ, Anderson BO, Blair SL, Burstein HJ, Cyr A, Elias AD, Farrar WB, Forero A, Giordano SH, Goldstein LJ, Hayes DF, Hudis CA, Isakoff SJ, Ljung BM, Marcom PK, Mayer IA, McCormick B, Miller RS, Pegram M, Pierce LJ, Reed EC, Salerno KE, Schwartzberg LS, Smith ML, Soliman H, Somlo G, Ward JH, Wolff AC, Zellars R, Shead DA, and Kumar R

Subjects

Female, Humans, Breast Neoplasms diagnosis, Breast Neoplasms therapy

Abstract

Breast cancer is the most common malignancy in women in the United States and is second only to lung cancer as a cause of cancer death. The overall management of breast cancer includes the treatment of local disease with surgery, radiation therapy, or both, and the treatment of systemic disease with cytotoxic chemotherapy, endocrine therapy, biologic therapy, or combinations of these. The NCCN Guidelines specific to management of large clinical stage II and III tumors are discussed in this article. These guidelines are the work of the members of the NCCN Breast Cancer Panel. Expert medical clinical judgment is required to apply these guidelines in the context of an individual patient to provide optimal care. Although not stated at every decision point of the guidelines, patient participation in prospective clinical trials is the preferred option of treatment for all stages of breast cancer.

Published

2014

25. Breast cancer, version 3.2013: featured updates to the NCCN guidelines.

Author

Theriault RL, Carlson RW, Allred C, Anderson BO, Burstein HJ, Edge SB, Farrar WB, Forero A, Giordano SH, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Isakoff SJ, Ljung BM, Mankoff DA, Marcom PK, Mayer IA, McCormick B, Pierce LJ, Reed EC, Schwartzberg LS, Smith ML, Soliman H, Somlo G, Ward JH, Wolff AC, Zellars R, Shead DA, and Kumar R

Subjects

Female, Humans, Molecular Targeted Therapy, Neoplasm Metastasis, Neoplasm Staging, Receptor, ErbB-2 antagonists & inhibitors, Receptor, ErbB-2 metabolism, Recurrence, Breast Neoplasms diagnosis, Breast Neoplasms drug therapy

Abstract

These NCCN Guidelines Insights highlight the important updates specific to the management of HER2-positive metastatic breast cancer in the 2013 version of the NCCN Clinical Practice Guidelines in Oncology for Breast Cancer. These include new first-line and subsequent therapy options for patients with HER2-positive metastatic breast cancer.

Published

2013

26. Metastatic breast cancer, version 1.2012: featured updates to the NCCN guidelines.

Author

Carlson RW, Allred DC, Anderson BO, Burstein HJ, Edge SB, Farrar WB, Forero A, Giordano SH, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Isakoff SJ, Ljung BM, Mankoff DA, Marcom PK, Mayer IA, McCormick B, Pierce LJ, Reed EC, Smith ML, Soliman H, Somlo G, Theriault RL, Ward JH, Wolff AC, Zellars R, Kumar R, and Shead DA

Subjects

Biomarkers, Tumor, Breast Neoplasms metabolism, Female, Humans, Neoplasm Metastasis, TOR Serine-Threonine Kinases antagonists & inhibitors, Antineoplastic Agents, Hormonal therapeutic use, Breast Neoplasms drug therapy, Breast Neoplasms pathology, Protein Kinase Inhibitors therapeutic use

Abstract

These NCCN Guidelines Insights highlight the important updates/changes specific to the management of metastatic breast cancer in the 2012 version of the NCCN Clinical Practice Guidelines in Oncology (NCCN Guidelines) for Breast Cancer. These changes/updates include the issue of retesting of biomarkers (estrogen receptor, progesterone receptor, and human epidermal growth factor receptor 2) on recurrent disease, new information regarding first-line combination endocrine therapy for metastatic disease, a new section on monitoring of patients with metastatic disease, and new information on endocrine therapy combined with an mTOR inhibitor as a subsequent therapeutic option.

Published

2012

27. Spirituality, patients' worry, and follow-up health-care utilization among cancer survivors.

Author

Cannon AJ, Darrington DL, Reed EC, and Loberiza FR Jr

Subjects

Adult, Aged, Female, Follow-Up Studies, Humans, Male, Middle Aged, Survivors, Anxiety Disorders epidemiology, Delivery of Health Care statistics & numerical data, Neoplasms psychology, Spirituality

Abstract

Background: Spirituality may aid cancer survivors as they attempt to interpret the meaning of their experience., Objective: We examined the relationship between spirituality, patient-rated worry, and health-care utilization among 551 cancer survivors with different malignancies, who were evaluated prospectively., Methods: Baseline spirituality scores were categorized into low and high spirituality groups. Patient-rated worries regarding disease recurrence/progression, developing new cancer, and developing complications from treatment were collected at baseline and at 6 and 12 months. Follow-up health-care utilization was also examined at 6 and 12 months., Results: Among the survivors, 271 (49%) reported low spirituality and 280 (51%) reported high spirituality. Of the cohort, 59% had some kind of worry regarding disease recurrence/progression, development of new cancers, and treatment complications. Highly spiritual survivors were less likely to have high levels of worries at both 6 and 12 months. Highly worried survivors were significantly more likely to place phone calls to their follow-up providers and had more frequent follow-up visits at 6 and 12 months. No interactions between spirituality and level of worry were noted to affect follow-up health-care utilization., Conclusion: Given spirituality's effect on anxiety, spirituality-based intervention may have a role in addressing cancer survivors' worries but may not improve health-care utilization.

Published

2011

28. Invasive breast cancer.

Author

Carlson RW, Allred DC, Anderson BO, Burstein HJ, Carter WB, Edge SB, Erban JK, Farrar WB, Forero A, Giordano SH, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Ljung BM, Mankoff DA, Marcom PK, Mayer IA, McCormick B, Pierce LJ, Reed EC, Sachdev J, Smith ML, Somlo G, Ward JH, Wolff AC, and Zellars R

Subjects

Female, Humans, Neoplasm Invasiveness, Risk Factors, Breast Neoplasms diagnosis, Breast Neoplasms drug therapy, Breast Neoplasms therapy

Published

2011

29. Breast cancer: noninvasive and special situations.

Author

Carlson RW, Allred DC, Anderson BO, Burstein HJ, Carter WB, Edge SB, Erban JK, Farrar WB, Forero A, Giordano SH, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Ljung BM, Marcom PK, Mayer IA, McCormick B, Pierce LJ, Reed EC, Smith ML, Somlo G, Topham NS, Ward JH, Winer EP, and Wolff AC

Subjects

Breast Neoplasms therapy, Carcinoma in Situ therapy, Carcinoma, Intraductal, Noninfiltrating therapy, Female, Humans, Neoplasm Staging, Breast Neoplasms pathology, Carcinoma in Situ pathology, Carcinoma, Intraductal, Noninfiltrating pathology

Published

2010

30. Breast cancer. Clinical practice guidelines in oncology.

Author

Carlson RW, Allred DC, Anderson BO, Burstein HJ, Carter WB, Edge SB, Erban JK, Farrar WB, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Jahanzeb M, Kiel K, Ljung BM, Marcom PK, Mayer IA, McCormick B, Nabell LM, Pierce LJ, Reed EC, Smith ML, Somlo G, Theriault RL, Topham NS, Ward JH, Winer EP, and Wolff AC

Subjects

Algorithms, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized, Aromatase Inhibitors therapeutic use, Breast radiation effects, Breast Neoplasms drug therapy, Breast Neoplasms metabolism, Breast Neoplasms mortality, Breast Neoplasms pathology, Breast Neoplasms surgery, Combined Modality Therapy, Female, Humans, Lymphatic Metastasis, Mastectomy, Neoadjuvant Therapy, Neoplasm Invasiveness, Neoplasm Recurrence, Local prevention & control, Neoplasm Staging, Neoplasms, Hormone-Dependent drug therapy, Neoplasms, Hormone-Dependent metabolism, Postmenopause, Premenopause, Randomized Controlled Trials as Topic, Receptor, ErbB-2 metabolism, Selective Estrogen Receptor Modulators therapeutic use, Sentinel Lymph Node Biopsy, Tamoxifen therapeutic use, Trastuzumab, Breast Neoplasms therapy

Published

2009

31. Tumor and iatrogenic regulation of myeloid precursors and their potential to limit immune therapy.

Author

Talmadge JE, Cowan KH, and Reed EC

Subjects

Animals, Cytokines immunology, Cytokines metabolism, Humans, Immunosuppression Therapy adverse effects, Myeloid Progenitor Cells pathology, Neoplasms pathology, Tumor Escape, Immunotherapy trends, Myeloid Progenitor Cells immunology, Neoplasms immunology

Published

2009

32. Invasive breast cancer.

Author

Carlson RW, Anderson BO, Burstein HJ, Carter WB, Edge SB, Farrar WB, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis CA, Jahanzeb M, Ljung BM, Kiel K, Marks LB, McCormick B, Nabell LM, Pierce LJ, Reed EC, Silver SM, Smith ML, Somlo G, Theriault RL, Ward JH, Winer EP, and Wolff AC

Subjects

Antineoplastic Agents therapeutic use, Breast Neoplasms therapy, Carcinoma, Ductal, Breast therapy, Carcinoma, Lobular therapy, Chemotherapy, Adjuvant, Female, Humans, Mastectomy, Mastectomy, Segmental, Neoplasm Invasiveness, Neoplasm Staging, Practice Guidelines as Topic, Radiotherapy, Breast Neoplasms pathology, Carcinoma, Ductal, Breast pathology, Carcinoma, Lobular pathology

Published

2007

33. Effect of diabetes mellitus on the epidemiology and outcomes of colon cancer.

Author

Shonka NA, Anderson JR, Panwalkar AW, Reed EC, Steen PD, and Ganti AK

Subjects

Age Factors, Aged, Aged, 80 and over, Female, Humans, Male, Middle Aged, Prognosis, Retrospective Studies, Sex Factors, Survival Analysis, Colonic Neoplasms complications, Colonic Neoplasms epidemiology, Diabetes Complications epidemiology, Diabetes Mellitus epidemiology

Abstract

Objectives: To assess the effect of diabetes mellitus (DM) on the pathogenesis and outcomes from colon cancer., Methods: A retrospective chart review was conducted on 1853 patients with colon cancer., Results: A higher percentage of males than females with colon cancer had DM (16.2% vs 11.3%; p < 0.01). Males had a slightly lower risk of dying from colon cancer (RR - 0.88; p=0.08). There was no difference in the median age of diagnosis of colon cancer in patients with and without DM, but a larger proportion of patients with diabetes mellitus were >or=70 yr at diagnosis (50% vs 43%) (p=0.0004). No significant relationship was noted between stage of colon cancer or survival and presence of DM., Conclusions: DM did not affect either the stage at diagnosis, or outcomes from colon cancer. More males with colon cancer tended to have DM and a larger proportion of patients with DM were >or=70 yr at the time of diagnosis.

Published

2006

34. Breast cancer.

Author

Carlson RW, Anderson BO, Burstein HJ, Cox CE, Edge SB, Farrar WB, Goldstein LJ, Gradishar WJ, Hayes DF, Hudis C, Jahanzeb M, Ljung BM, Marks LB, McCormick B, Nabell LM, Pierce LJ, Reed EC, Silver SM, Smith ML, Somlo G, Theriault RL, Ward JH, Winer EP, and Wolff AC

Subjects

Antineoplastic Agents therapeutic use, Breast Neoplasms diagnosis, Combined Modality Therapy, Female, Humans, Mammography, Mastectomy, Neoplasm Staging, Radiotherapy, Adjuvant, Biomarkers, Tumor, Breast Neoplasms therapy

Published

2005

35. Cigarette smoke extract inhibits chemotaxis and collagen gel contraction mediated by human bone marrow osteoprogenitor cells and osteoblast-like cells.

Author

Liu X, Kohyama T, Kobayashi T, Abe S, Kim HJ, Reed EC, and Rennard SI

Subjects

Becaplermin, Bone Remodeling physiology, Cell Differentiation physiology, Cell Migration Inhibition, Cells, Cultured, Chemotactic Factors physiology, Collagen, Fibronectins biosynthesis, Fibronectins physiology, Gels, Humans, Platelet-Derived Growth Factor physiology, Proto-Oncogene Proteins c-sis, Smoking adverse effects, Transforming Growth Factor beta physiology, Transforming Growth Factor beta1, Bone Marrow Cells physiology, Osteoblasts physiology, Smoke adverse effects, Stem Cells physiology, Nicotiana adverse effects

Abstract

Cell migration and matrix remodeling are key events in tissue repair and restructuring. Osteoblasts are responsible for the production of new bone matrix during bone remodeling. The activity of these cells can be modulated by a number of factors. The current study evaluated the hypothesis that cigarette smoke extract can alter repair and remodeling responses of human osteoprogenitor cells and osteoblast-like cells and, therefore, could explain one mechanism by which cigarette smoking leads to osteoporosis. Human osteoprogenitor cells were isolated from normal human bone marrow and maintained in culture under either control conditions or conditions that induced differentiation into osteoblast-like cells. Both cell types migrated toward fibronectin and PDGF-BB as chemoattractants. Neither responded to TGF-beta1. The osteoprogenitor cells were more active in their chemotactic response. The chemotactic response of both cell types was inhibited by cigarette smoke extract in a concentration-dependent manner. Both cell types, when cultured in three-dimensional native collagen gels maintained in floating culture, induced contraction of their surrounding matrices. Contraction was augmented by serum, PDGF-BB, and TGF-beta1. Osteoprogenitor cells were less active in inducing contraction than were osteoblast-like cells. Contraction of both cell types was inhibited by cigarette smoke extract. Cigarette smoke extract also inhibited the production of fibronectin by both cell types maintained in three-dimensional culture. Addition of exogenous fibronectin partially restored the ability of the cells to contract three-dimensional collagen gels. The current study demonstrates that cigarette smoke can interfere with the ability of bone cells to participate in repair and remodeling events. Such an effect may be one mechanism leading to the development of osteoporosis.

Published

2003

36. Optimal multidimensional bit-rate control for video communication.

Author

Reed EC and Lim JS

Abstract

In conventional bit-rate control, the buffer level is controlled by adapting the quantization step size with a fixed frame rate and spatial resolution. We consider a multidimensional (M-D) bit-rate control where the frame rate, spatial resolution and quantization step size are jointly adapted for buffer control. We introduce a fundamental framework to formalize the description of the M-D buffer-constrained allocation problem. Given a set of operating points on a M-D grid to code a nonstationary source in a buffer-constrained environment, we formulate the optimal solution. The formulation allows a skipped frame to be reconstructed from one coded frame using any temporal interpolation method and is shown to be a generalization of formulations considered in the literature. In the case of intraframe coding, a dynamic programming algorithm is introduced to find the optimal solution. The algorithm allows one to compare operational rate-distortion bounds of the M-D and conventional approaches. We also discuss how a solution can be obtained for the case of interframe coding using the optimal dynamic programming algorithm for intraframe coding by making an independent allocation approximation. We illustrate that the M-D approach can provide bit-rate reductions over 50%. We also show that the M-D approach with limited-lookahead provides a slightly suboptimal solution that consistently outperforms the conventional approach with full-lookahead.

Published

2002

37. NCCN Practice Guidelines for Breast Cancer.

Author

Carlson RW, Anderson BO, Bensinger W, Cox CE, Davidson NE, Edge SB, Farrar WB, Goldstein LJ, Gradishar WJ, Lichter AS, McCormick B, Nabell LM, Reed EC, Silver SM, Smith ML, Somlo G, Theriault R, Ward JH, Winer EP, and Wolff A

Subjects

Breast Neoplasms classification, Female, Follow-Up Studies, Humans, Lymph Node Excision, Lymphatic Metastasis, Neoplasm Metastasis, Neoplasm Recurrence, Local, Neoplasm Staging, Risk Management, Breast Neoplasms pathology, Breast Neoplasms therapy

Abstract

The therapeutic options for patients with noninvasive or invasive breast cancer are complex and varied. In many situations, the patient and physician have the responsibility to jointly explore and ultimately select the most appropriate option from among the available alternatives. With rare exception, the evaluation, treatment, and follow-up recommendations contained within these guidelines were based largely on the results of past and present clinical trials. However, there is not a single clinical situation in which the treatment of breast cancer has been optimized with respect to either maximizing cure or minimizing toxicity and disfigurement. Therefore, patient and physician participation in prospective clinical trials allows patients not only to receive state-of-the-art cancer treatment but also to contribute to the improvement of treatment of future patients.

Published

2000

38. Invasive pulmonary aspergillosis due to Aspergillus terreus: 12-year experience and review of the literature.

Author

Iwen PC, Rupp ME, Langnas AN, Reed EC, and Hinrichs SH

Subjects

Antifungal Agents therapeutic use, Aspergillosis drug therapy, Female, Humans, Immunocompromised Host, Lung Diseases, Fungal drug therapy, Male, Neutropenia complications, Peritoneal Diseases drug therapy, Retrospective Studies, Transplantation, Aspergillosis microbiology, Aspergillus isolation & purification, Lung Diseases, Fungal microbiology, Peritoneal Diseases microbiology

Abstract

A 12-year retrospective analysis was done to identify and evaluate in detail cases of invasive pulmonary aspergillosis (IPA) caused by Aspergillus terreus. We identified 13 A. terreus infections among 133 total cases of confirmed invasive aspergillosis; 11 were IPA and 2 were primary peritoneal infections. Of the 11 patients with IPA, 7 developed neutropenia during hospitalization, and the remaining four were receiving immunosuppressive agents. Ten patients with IPA died; one liver transplantation patient without neutropenia survived after treatment with amphotericin B, itraconazole, and a pulmonary lobectomy. Six patients developed disseminated disease, with the heart the most common extrapulmonary site identified (four patients). These cases demonstrate that IPA caused by A. terreus rapidly progresses in immunocompromised patients receiving amphotericin B and illustrate the need for sensitive diagnostic tests and more effective antifungal agents.

Published

1998

39. Hematopoietic recovery after allogeneic blood stem-cell transplantation compared with bone marrow transplantation in patients with hematologic malignancies.

Author

Pavletic ZS, Bishop MR, Tarantolo SR, Martin-Algarra S, Bierman PJ, Vose JM, Reed EC, Gross TG, Kollath J, Nasrati K, Jackson JD, Armitage JO, and Kessinger A

Subjects

Adult, Female, Granulocyte Colony-Stimulating Factor, Humans, Male, Middle Aged, Survival Analysis, Tissue Donors, Transplantation, Homologous, Treatment Outcome, Bone Marrow Transplantation, Hematologic Neoplasms physiopathology, Hematologic Neoplasms surgery, Hematopoiesis, Hematopoietic Stem Cell Transplantation

Abstract

Purpose: To compare hematopoietic recovery, duration of hospitalization, and 100-day survival in patients who received allogeneic-blood stem cells (BSC) or conventional allogeneic bone marrow transplantation (BMT)., Patients and Methods: From December 1994 to August 1995, 21 patients participated in a phase II study of allogeneic BSC transplantation. Cells mobilized with granulocyte colony-stimulating factor (G-CSF; 5 micrograms/kg/ d) were collected from human leukocyte antigen (HLA)-matched related donors and cryopreserved. Graft-versus-host disease (GVHD) prophylaxis consisted of cyclosporine and methotrexate. G-CSF (10 micrograms/kg/d) was administered posttransplant. The outcomes were compared with 22 identically treated historical patients who received allogeneic BMT., Results: The median infused CD34+ cell and granulocyte-macrophage colony-forming unit (CFU-GM) content were 7.73 x 10(4)/kg and 41.6 x 10(4)/kg, respectively. The median time to a neutrophil count greater than 500/ microL was 11 days after BSC and 16.5 days after BMT (P = .0003). A trend toward faster platelet and RBC recovery after BSC was observed. BSC patients received fewer platelet transfusions: 10 versus 19 (P = .015). The median length of hospitalization was shorter after BSC transplantation: 25 versus 31.5 days (P = .0243). The 100-day survival rates were similar: 83% after BSC and 75% after BMT (P = .3585). The incidence of acute GVHD grade II to IV was 57% and 45% for BSC and BMT, respectively (P = .4654)., Conclusion: In comparison to BMT, allogeneic BSC transplantation may result in faster hematopoietic recovery, shorter hospital stay, and similar early survival. Whether allogeneic BSC are superior to bone marrow needs to be determined in randomized trials.

Published

1997

40. Immunologic phenotype and function in human bone marrow, blood stem cells and umbilical cord blood.

Author

Mills KC, Gross TG, Varney ML, Heimann DG, Reed EC, Kessinger A, and Talmadge JE

Subjects

Bone Marrow drug effects, Bone Marrow pathology, Bone Marrow Cells, Breast Neoplasms immunology, Breast Neoplasms pathology, Cytotoxicity, Immunologic, Female, Fetal Blood cytology, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Humans, Immunophenotyping, Killer Cells, Natural immunology, Leukapheresis, Lymphocyte Activation drug effects, Lymphocyte Count, Lymphoma immunology, Lymphoma pathology, Male, Mitogens pharmacology, Receptors, Antigen, T-Cell, gamma-delta analysis, T-Lymphocytes, Regulatory drug effects, T-Lymphocytes, Regulatory immunology, Bone Marrow immunology, Fetal Blood immunology, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells immunology, Lymphocyte Subsets immunology

Abstract

The T cell-mediated antineoplastic activity observed following allogeneic transplantation and the suggestion of improved therapeutic efficacy by autologous peripheral stem cell transplantation (PSCT) as compared to autologous bone marrow transplantation (ABMT) for non-Hodgkin's lymphoma (NHL) stimulated our interest in the immunologic competence of stem cell products. We report the immune phenotype and function of normal peripheral blood (PB) cells, bone marrow (BM) cells from normal donors and cancer bearing patients, GM-CSF-mobilized and apheresed blood mononuclear cells from NHL patients, unmobilized apheresed mononuclear cells from normal volunteers and umbilical cord blood (CB). The analyses include three-color fluorescent cytometry of the major hematologic and immunologic phenotypes as well as natural killer (NK) activity, natural suppressor (NS) activity, and phytohemagglutinin (PHA) and pokeweed (PWM) mitogenesis. These studies demonstrated an increased frequency of T cells in apheresis products as compared to BM and CB products. Specifically, the mobilized PSC had significant increases in CD3+, CD4+, CD45RO+ and CD56+ cells relative to BM cells. In addition, the frequency of TCR gamma/delta + cells in all the stem cell products, with the exception of CB, were also increased compared to normal peripheral blood leukocytes (PBL). However, all the stem cell products had a significant depression in T (PHA mitogenesis) and B (PWM mitogenesis) cell function. The depression in immune cell functionality, in the PSC products was perhaps due to the high frequency of monocytes which appeared to be increased due to both mobilization and apheresis. The frequency of the NK cell phenotype (CD56) but not function was increased in the mobilized PSC products, while the NK cell function in the BM products from cancer patients but not normal donors was depressed as compared to normal PBL. In summary, there are significant differences in the cellular phenotypes and immunologic competence among the various stem cell products with potential therapeutic implications.

Published

1996

41. Use of continuous infusion granulocyte-macrophage colony-stimulating factor alone or followed by granulocyte colony-stimulating factor to enhance engraftment following high-dose chemotherapy and autologous bone marrow transplantation for lymphoid malignancies.

Author

Vose JM, Bierman PJ, Ruby E, Reed EC, Bishop MR, Tarantolo S, Kessinger A, and Armitage JO

Subjects

Adult, Combined Modality Therapy, Female, Granulocyte Colony-Stimulating Factor adverse effects, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage, Granulocyte-Macrophage Colony-Stimulating Factor adverse effects, Humans, Lymphoma blood, Male, Transplantation, Autologous, Antineoplastic Agents therapeutic use, Bone Marrow Transplantation, Granulocyte Colony-Stimulating Factor administration & dosage, Granulocyte-Macrophage Colony-Stimulating Factor therapeutic use, Lymphoma therapy

Abstract

We evaluated the differences in engraftment and toxicities post-autologous transplant using granulocyte-macrophage colony stimulating factor (GM-CSF) as a continuous infusion either alone or in a sequential manner with granulocyte colony-stimulating factor (G-CSF). Patients receiving high-dose chemotherapy and autologous bone marrow transplantation (ABMT) for lymphoid malignancies participated in two phase II trials evaluating either continuous infusion GM-CSF (GM-CSF (CI)) or continuous infusion GM-CSF followed by sequential G-CSF (GM-CSF/G-CSF) administered post-ABMT. These patients were compared to similar historical control patients receiving GM-CSF administered as a 2-h intravenous (i.v.) infusion (GM-CSF (2-h)). Patients receiving GM-CSF (CI) and GM-CSF/G-CSF had a median day to reach an absolute neutrophil count of 500/microliter post-ABMT of 12 and 11 days, respectively. This compared to a median day of 22 in the GM-CSF (2-h) historical control patients. The median day to platelet independence was 18, 18 and 30 days, respectively. The incidence of toxicities such as incidence of infection, pleural effusions, and rash did not differ greatly between the groups. We conclude that the use of continuous infusion GM-CSF either alone or sequentially with G-CSF produced improved engraftment times compared to historical control patients treated with GM-CSF as a 2-h i.v. infusion. The toxicities at a reduced dose of 125 micrograms/m2 given as a continuous infusion appear to be similar to those seen in patients receiving GM-CSF as a 2-h infusion.

Published

1996

42. Systemic adjuvant therapy for breast cancer.

Author

Reed EC

Subjects

Adult, Chemotherapy, Adjuvant adverse effects, Female, Humans, Middle Aged, Patient Selection, Prognosis, Antineoplastic Agents, Hormonal therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Breast Neoplasms drug therapy, Tamoxifen therapeutic use

Abstract

The benefits of adjuvant systemic therapy in the treatment of early breast cancer are well established. However, many questions remain regarding the appropriate selection of patients and regimens, duration of treatment, timing or sequencing of treatment as well as the role of high-dose chemotherapy or new active drugs such as paclitaxel. Future answers will only come through continued participation in carefully designed clinical research.

Published

1996

43. Immunologic attributes of cytokine mobilized peripheral blood stem cells and recovery following transplantation.

Author

Talmadge JE, Reed EC, Kessinger A, Kuszynski CA, Perry GA, Gordy CL, Mills KC, Thomas ML, Pirruccello SJ, Letheby BA, Arneson MA, and Jackson JD

Subjects

Antigens, CD34 analysis, CD4 Antigens analysis, CD8 Antigens analysis, Hematopoietic Stem Cells drug effects, Humans, Immunophenotyping, Killer Cells, Natural immunology, Lymphocyte Activation, T-Lymphocytes, Regulatory immunology, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Hematopoietic Stem Cell Transplantation, Hematopoietic Stem Cells immunology

Abstract

The immunologic attributes of cytokine mobilized peripheral blood stem cell (PSC) products (n = 52) and the resulting reconstitution of the hematopoietic and immunologic system following autologous transplantation were examined in a consecutive population of non-Hodgkin lymphoma (NHL), or solid tumor patients at the University of Nebraska Medical Center. Granulocyte-monocyte colony stimulating factor (GM-CSF)-mobilized PSC products had a high frequency of monocytes (31%) and bands (15%) as compared to normal peripheral blood (PB) cells. The phenotypic analysis of the mobilized PSC product revealed that they had normal levels of CD4+ cells, an increased frequency of CD8+ cells and a corresponding decrease in the CD4+:CD8+ cell ratio as compared to the peripheral blood leukocytes (PBL) of normal individuals. PSC products also had an increase in CD34+ cells as compared to PB. Natural killer (NK) and T cell activity in the PSC products were also lower than that observed in PB. Post-transplantation there was an accelerated reconstitution of NK-cell function in the PB as compared to T cell function (PHA (phytohemagglutinin) mitogenesis) which did not return to normal by day 100 post-transplantation. We also report for the first time high levels of an irradiation resistant suppressor cell activity in the PSC product and in the PB post-transplantation. There was also a concomitant increase in CD4-, CD8-, TCR alpha/beta+ cells (phenotypic homolog of 'natural suppressor' (NS) cells) in the PB post-transplantation. The number of months of prior chemotherapy correlated with PHA response but the NS activity and frequency of CD4-, CD8- and TCR alpha/beta+ cells did not. Further, cytokine mobilization and apheresis appears to contribute to the loss of PHA responsiveness and the increased levels of suppressor cell activity.

Published

1996

44. Multiple organ dysfunction syndrome in bone marrow transplantation.

Author

Haire WD, Ruby EI, Gordon BG, Patil KD, Stephens LC, Kotulak GD, Reed EC, Vose JM, Bierman PJ, and Kessinger A

Subjects

Adolescent, Adult, Aged, Analysis of Variance, Biomarkers blood, Bone Marrow Transplantation mortality, Bone Marrow Transplantation physiology, Cohort Studies, Female, Humans, Logistic Models, Male, Middle Aged, Multiple Organ Failure blood, Multiple Organ Failure mortality, Proportional Hazards Models, Survival Analysis, Antithrombin III metabolism, Bone Marrow Transplantation adverse effects, Multiple Organ Failure etiology, Protein C metabolism

Abstract

Objective: To define the frequency and outcome of organ dysfunction in bone marrow transplantation (BMT) and to determine if patients with organ dysfunction have lower levels of protein C (PC) and/or antithrombin III (ATIII) than those without organ dysfunction., Design: Inception cohort of patients undergoing BMT, followed for 28 days, until hospital dismissal, or until death., Setting: Bone marrow transplant department of a university hospital., Patients: A total of 199 consecutive patients admitted for BMT., Interventions: Standard supportive care was given to all patients., Main Outcome Measures: Definitions of organ dysfunction were arrived at prior to beginning the study. They include pulmonary, central nervous system (CNS), hepatic, and renal dysfunction. Protein C and ATIII levels were measured prior to beginning the preparative regimen and weekly thereafter., Results: Single organ dysfunction, manifesting as pulmonary, CNS, or hepatic dysfunction, occurred in 93 (48.5%) of the 199 patients and was a strong predictor of multiple organ dysfunction syndrome (MODS) and death. Death occurred in 14 (7.0%) of the patients. Cause of death was precisely identified in only four patients. Low levels of either PC or ATIII were associated with death and pulmonary, CNS, and hepatic dysfunction. Multivariate analysis showed ATIII and PC levels were associated with single organ dysfunction independent of the type of transplant, the type of preparative regimen, and the presence of bacteremia., Conclusions: Single organ dysfunction during BMT is a marker for a systemic abnormality that has a high likelihood of progressing to MODS, similar to that seen in other critically ill patient populations. MODS is the leading cause of death in series of BMT patients. Low levels of ATIII and PC are markers of and may be involved in the pathogenesis of MODS in BMT.

Published

1995

45. Erythropoietin for mobilization of circulating progenitor cells in patients with previously treated relapsed malignancies.

Author

Kessinger A, Bishop MR, Jackson JD, O'Kane-Murphy B, Vose JM, Bierman PJ, Reed EC, Warkentin PI, Armitage JO, and Sharp JG

Subjects

Adult, Aged, Cells, Cultured, Combined Modality Therapy, Erythropoietin pharmacology, Female, Hematopoietic Stem Cell Transplantation, Humans, Male, Middle Aged, Neoplasm Recurrence, Local, Recombinant Proteins administration & dosage, Recombinant Proteins pharmacology, Erythropoietin administration & dosage, Hematopoietic Stem Cells drug effects, Immunotherapy, Adoptive, Neoplasms therapy

Abstract

A trial to determine the usefulness of recombinant human erythropoietin (rhEpo) as a mobilizing cytokine for patients with previously treated relapsed malignancies was performed. An initial peripheral stem cell apheresis collection was conducted during steady-state hematopoiesis for each patient to provide baseline data. rhEpo, 200 U/kg/day, was administered subcutaneously until the last apheresis procedure was completed. Immediately after the fourth daily dose of Epo, apheresis procedures were resumed and continued beyond five collections, when necessary, to accrue a total of 6.5 x 10(8) mononuclear cells (MNCs)/kg. Eight female and four male patients (median age = 44 years) were evaluated. Five to 14 (median = 8) apheresis procedures were performed for each patient. Toxicity attributable to Epo administration was negligible. Mobilization effects, as determined by an increase in the number of colony-forming units granulocyte/macrophage (CFU-GM) and burst-forming units-erythroid (BFU-E) in the apheresis products after Epo administration, were observed in all patients. Nine patients received high-dose chemotherapy and Epo-mobilized peripheral stem cell transplantation (PSCT). Beginning the day of the transplant, GM-CSF was administered until neutrophil recovery was satisfactory. The median time to recover 0.5 x 10(9)/L granulocytes was 16 days after PSCT. Epo appears to have mobilization properties. Further studies are needed to determine the clinical usefulness of Epo as a mobilizing cytokine. The addition of Epo to other mobilizing cytokines may provide increased effectiveness without adding toxicity.

Published

1995

46. Pulmonary resection for invasive Aspergillus infections in immunocompromised patients.

Author

Robinson LA, Reed EC, Galbraith TA, Alonso A, Moulton AL, and Fleming WH

Subjects

Adult, Amphotericin B therapeutic use, Antifungal Agents therapeutic use, Aspergillosis drug therapy, Aspergillosis immunology, Aspergillosis mortality, Female, Follow-Up Studies, Hospital Mortality, Humans, Lung diagnostic imaging, Lung Diseases, Fungal drug therapy, Lung Diseases, Fungal immunology, Lung Diseases, Fungal mortality, Male, Retrospective Studies, Time Factors, Tomography, X-Ray Computed, Aspergillosis surgery, Hematologic Diseases immunology, Immunocompromised Host, Liver Transplantation immunology, Lung Diseases, Fungal surgery, Pneumonectomy

Abstract

Standard antifungal medical therapy of invasive pulmonary aspergillosis that occurs in immunocompromised patients with hematologic diseases with neutropenia or in liver transplant recipients results in less than a 5% survival. In view of these dismal mortality rates, we adopted an aggressive approach with resection of the involved area of lung along with systemic antifungal therapy when localized invasive pulmonary aspergillosis developed in these patients. Between January 1987 and December 1993, 14 patients with hematologic diseases and 2 liver transplant recipients underwent resection of acute localized pulmonary masses suggestive of invasive pulmonary aspergillosis a median of 7.5 days (range 1 to 45 days) after the diagnosis was clinically suggested and confirmed by chest computed tomographic scans. Operative procedures done included two pneumonectomies, one bilobectomy with limited thoracoplasty, nine lobectomies, and five wedge resections (one patient with hematologic disease had two procedures). All patients were treated before and after the operation with antifungal agents. Nine (64%) of 14 patients with hematologic disease and 2 (100%) of 2 liver transplant recipients survived the hospitalization with no evidence of recurrent Aspergillus infection after a median 8 months of follow-up (range 3 to 82 months). The five hospital deaths (all patients with hematologic diseases) occurred a median of 20 days after operation from diffuse alveolar hemorrhage in three, graft-versus-host disease in one, and multiple organ system failure with presumed disseminated Aspergillus infection in one. Four of the five deaths were in patients with allogeneic bone marrow transplants. Two of the three patients requiring resection of multiple foci of infection died, as did the only patient who was preoperatively ventilator dependent. In immunocompromised patients with hematologic diseases or liver transplantation with invasive pulmonary aspergillosis, early pulmonary resection should be strongly considered when the characteristic clinical and radiographic pictures appear.

Published

1995

47. Comparison of subcutaneous and intravenous administration of recombinant human granulocyte-macrophage colony-stimulating factor for peripheral blood stem cell mobilization.

Author

Kessinger A, Bishop MR, Anderson JR, Armitage JO, Bierman PJ, Reed EC, Tarantolo S, Tempero MA, Vose JM, and Warkentin PI

Subjects

Adult, Aged, Cytapheresis, Female, Granulocyte Colony-Stimulating Factor pharmacology, Granulocyte-Macrophage Colony-Stimulating Factor pharmacology, Hematopoietic Stem Cell Transplantation, Humans, Infusions, Intravenous, Injections, Subcutaneous, Male, Middle Aged, Recombinant Fusion Proteins administration & dosage, Recombinant Fusion Proteins pharmacology, Granulocyte-Macrophage Colony-Stimulating Factor administration & dosage, Hematopoietic Stem Cells drug effects, Leukocytes, Mononuclear drug effects

Abstract

In an effort to determine whether subcutaneous or continuous intravenous infusion administration of rhGM-CSF results in better hematopoietic progenitor mobilization, the findings of two sequential clinical trials were reviewed. Patients who had received prior chemotherapy for leukemia, lymphoma, multiple myeloma, breast cancer, or other solid tumors and were candidates for high-dose therapy received rhGM-CSF, 250 micrograms/m2/day, either as a continuous intravenous infusion (trial 1) or subcutaneously (trial 2) for stem cell mobilization. At least five apheresis collection procedures were performed to collect a target number of 6.5 x 10(8) mononuclear cells (MNC)/kg. For the 37 patients in trial 1, the collections contained a median of 7.99 x 10(8) MNC/L (range 6.42-21.36) and a median of 5.27 x 10(4) CFU-GM/kg (range 0.28-19.35). In trial 1, 25 patients were autografted with their cells and recovered 0.5 x 10(9) granulocytes/L at a median of 12 days (range 6-16). For the 33 patients in trial 2, the autograft product contained a median of 7.63 x 10(8) MNC/kg (range 6.51-22.66) and 6.31 x 10(4) CFU-GM/kg (range 0.06-60.4). In trial 2, 25 patients were autografted. The median time to reach 0.5 x 10(9) granulocytes/L was 11 days (range 9-26). All patients received rhGM-CSF after peripheral stem cell transplant. No significant differences in the collected products or the time to hematopoietic recovery was found between the two trials (p > 0.05). The mobilization effects of subcutaneous rhGM-CSF in these pretreated patients were similar to those of intravenous rhGM-CSF.

Published

1995

48. Invasive infection due to Candida krusei in immunocompromised patients not treated with fluconazole.

Author

Iwen PC, Kelly DM, Reed EC, and Hinrichs SH

Subjects

Abdominal Injuries complications, Abdominal Injuries immunology, Adult, Aged, Breast Neoplasms complications, Breast Neoplasms immunology, Child, Child, Preschool, Female, Humans, Leukemia complications, Leukemia immunology, Liver Diseases complications, Liver Diseases immunology, Male, Middle Aged, Retrospective Studies, Candidiasis etiology, Fluconazole therapeutic use, Immunocompromised Host

Abstract

Candida krusei is a cause of invasive candidiasis (IC), with numerous cases reported among leukemia patients after bone marrow transplantation and treatment with fluconazole. The relation between fluconazole therapy and IC remains controversial. In a retrospective review covering 5 years, we identified 203 cases of IC, 71 (35%) of which were due to non-albicans species. Eight cases were caused by C. krusei: four of the patients involved had leukemia, two had breast cancer, one had end-stage liver disease, and one had undergone abdominal trauma. None of these patients received fluconazole. Surveillance cultures detected colonization with C. krusei before the onset of symptoms in seven cases. The median time from colonization to IC diagnosis was 10 days. Of six patients with neutropenia, five were neutropenic at IC diagnosis. Concomitant infections were common; four patients had both bacteremia and invasive aspergillosis. C. krusei was considered the immediate cause of five of the seven deaths among this group of patients. These eight cases extend the range of immunocompromised conditions in which IC caused by C. krusei develops in the absence of fluconazole therapy.

Published

1995

49. Incidence and characterization of secondary myelodysplastic syndrome and acute myelogenous leukemia following high-dose chemoradiotherapy and autologous stem-cell transplantation for lymphoid malignancies.

Author

Darrington DL, Vose JM, Anderson JR, Bierman PJ, Bishop MR, Chan WC, Morris ME, Reed EC, Sanger WG, and Tarantolo SR

Subjects

Adult, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Case-Control Studies, Cohort Studies, Combined Modality Therapy, Female, Hodgkin Disease mortality, Humans, Incidence, Leukemia, Myeloid, Acute epidemiology, Lymphoma, Non-Hodgkin mortality, Male, Middle Aged, Myelodysplastic Syndromes epidemiology, Prognosis, Radiotherapy Dosage, Risk Factors, Survival Rate, Whole-Body Irradiation, Bone Marrow Transplantation adverse effects, Hematopoietic Stem Cell Transplantation adverse effects, Hodgkin Disease therapy, Leukemia, Myeloid, Acute etiology, Lymphoma, Non-Hodgkin therapy, Myelodysplastic Syndromes etiology

Abstract

Purpose: To analyze the risk of developing myelodysplastic syndrome (MDS) or acute myelogenous leukemia (AML) following autologous bone marrow transplantation (ABMT) or peripheral stem-cell transplantation (PSCT) and to determine the impact on failure-free survival (FFS)., Patients and Methods: Patients underwent ABMT or PSCT for the treatment of Hodgkin's disease (HD) and non-Hodgkin's lymphoma (NHL) at the University of Nebraska Medical Center. For those patients who went on to develop MDS/AML, controls were selected and a case-control-within-a-cohort study undertaken., Results: Twelve patients developed MDS or AML a median of 44 months following ABMT/PSCT. The cumulative incidence (P = .42) and the conditional probability (P = .32) of MDS/AML were not statistically different between HD and NHL patients. Age greater than 40 years at the time of transplant (P = .05) and receipt of a total-body irradiation (TBI)-containing regimen (P = .06) were predictive for developing MDS/AML in patients with NHL., Conclusion: There is an increased risk of MDS/AML following ABMT/PSCT for lymphoid malignancies. NHL patients age > or = 40 years at the time of transplant and who received TBI are at greatest risk.

Published

1994

50. Airborne fungal spore monitoring in a protective environment during hospital construction, and correlation with an outbreak of invasive aspergillosis.

Author

Iwen PC, Davis JC, Reed EC, Winfield BA, and Hinrichs SH

Subjects

Environmental Monitoring, Epidemiological Monitoring, Hospital Units, Humans, Infection Control, Nebraska epidemiology, Prospective Studies, Air Microbiology, Aspergillosis epidemiology, Aspergillus flavus isolation & purification, Aspergillus fumigatus isolation & purification, Disease Outbreaks statistics & numerical data, Hospital Design and Construction, Neutropenia complications

Abstract

Objective: Evaluate aerobiological monitoring for fungal spores during hospital construction and correlate results with an outbreak of invasive aspergillosis (IA)., Design: Prospective air sampling for molds was done using the gravity air-settling plate (GASP) method., Setting: A university medical center special care unit consisting of single-patient rooms with high-efficiency particulate air filtration under positive pressure., Patients: Five neutropenic patients who subsequently developed IA., Results: Four of the five patients with IA were housed in rooms adjacent to a construction staging area. Aerobiological monitoring detected an increase in the number of airborne fungal spores including Aspergillus species in these rooms; however, increased counts preceded IA diagnosis by 1 to 7 days in only three of the five patients. Swab cultures of the exhaust vents within each room confirmed results from air-settling plates. Follow-up monitoring, using the GASP method, demonstrated that control procedures were effective in reducing air mold contamination., Conclusion: The GASP method, although able to demonstrate that infection control measures reduced mold contamination of the air, was insensitive to detect levels of mold contaminates in time to prevent IA.

Published

1994